Juan Santiago
Professor of Mechanical Engineering
Bio
Professor Santiago's research focuses on the study of microscale transport phenomena including electrokinetic flow, electrohydrodynamic instabilities, and general convective-diffusion-electromigration processes. His research includes the optimization and development of novel micro- and nano-devices for pumping liquids, on-chip electrophoresis, sample preconcentration methods, and miniature fuel cells. The applications of this work include microfabricated bioanalytical systems for genetic analysis, drug discovery, bioweapon detection, drug delivery, and power generation.
Academic Appointments
-
Professor, Mechanical Engineering
-
Member, Bio-X
-
Faculty Fellow, Stanford ChEM-H
Honors & Awards
-
Fellow, American Society of Mechanical Engineering (2012)
-
Fellow, American Physical Society (2010)
-
Outstanding Alumnus Award, Mechanical Engineering Department of the University of Florida (2008)
-
Outstanding Achievement in Academia Award, GEM Consortium (2006)
-
Presidential Early Career Award for Scientist and Engineers, PECASE (2004)
-
National Science Foundation Early Career Development (CAREER) Award, NSF (2003)
-
Collegiate Inventors Award, National Inventors Hall of Fame (2001)
-
Frederick Emmons Terman Fellow (Faculty) Award, Stanford University (1998)
-
Post-Doctoral Fellowship, Ford Foundation (1997)
Professional Education
-
PhD, University of Illinois at Urbana-Champaign (1995)
-
MS, University of Illinois at Urbana-Champaign (1992)
Current Research and Scholarly Interests
http://microfluidics.stanford.edu/Projects/Projects.html
2015-16 Courses
- Experimental Methods in Fluid Mechanics
ME 354 (Win) - Fluid Flow in Microdevices
ME 457 (Spr) - The Great Principle of Similitude
ME 13N (Aut) -
Independent Studies (7)
- Engineering Problems
ME 391 (Aut, Win, Spr, Sum) - Engineering Problems and Experimental Investigation
ME 191 (Aut, Win, Spr, Sum) - Experimental Investigation of Engineering Problems
ME 392 (Aut, Win, Spr, Sum) - Honors Research
ME 191H (Aut, Win, Spr, Sum) - Ph.D. Teaching Experience
ME 491 (Aut, Win, Spr, Sum) - Practical Training
ME 299A (Aut, Win, Spr, Sum) - Practical Training
ME 299B (Aut, Win, Spr, Sum)
- Engineering Problems
-
Prior Year Courses
2014-15 Courses
- Advanced Topics in Electrokinetics
ME 458 (Spr) - The Great Principle of Similitude
ME 13N (Aut)
2013-14 Courses
- Advanced Topics in Electrokinetics
ME 458 (Spr) - Experimental Methods in Fluid Mechanics
ME 354 (Aut) - Fluid Flow in Microdevices
ME 457 (Spr)
2012-13 Courses
- Experimental Methods in Fluid Mechanics
ME 354 (Aut) - Fluid Flow in Microdevices
ME 457 (Spr)
- Advanced Topics in Electrokinetics
All Publications
-
Rapid Slow Off-Rate Modified Aptamer (SOMAmer)-Based Detection of C-Reactive Protein Using Isotachophoresis and an Ionic Spacer
ANALYTICAL CHEMISTRY
2015; 87 (13): 6736-6743
Abstract
We present an on-chip electrophoretic assay for rapid protein detection with a SOMAmer (Slow Off-Rate Modified Aptamer) reagent. We used isotachophoresis (ITP) coupled with an ionic spacer to both react and separate SOMAmer-protein complex from free SOMAmer reagent. ITP accelerates the reaction kinetics as the ionic spacer concurrently separates the reaction products. We developed a numerical and analytical model to describe ITP spacer assays, which involve low-mobility, nonfocusing targets that are recruited into the ITP zone by higher-mobility, ITP-focused probes. We demonstrated a proof-of-concept of this assay using C-reactive protein (CRP) in buffer, and achieved a 2 nM limit of detection (LOD) with a combined 20 min assay time (10 min off-chip preparation of reagents and 10 min on-chip run). Our findings suggest that this approach has potential as a simple and rapid alternative to other homogeneous immunoassays. We also explore the extension of this assay to a diluted serum sample spiked with CRP, where we observe decreased sensitivity (an LOD of 25 nM in 20-fold diluted serum). We describe the challenges in extending this assay to complex samples and achieving higher sensitivity and specificity for clinical applications.
View details for DOI 10.1021/acs.analchem.5b00886
View details for Web of Science ID 000357839700048
-
Isotachophoresis for fractionation and recovery of cytoplasmic RNA and nucleus from single cells
ELECTROPHORESIS
2015; 36 (14): 1658-1662
Abstract
There is a substantial need for simultaneous analyses of RNA and DNA from individual single cells. Such analysis provides unique evidence of cell-to-cell differences and the correlation between gene expression and genomic mutation in highly heterogeneous cell populations. We present a novel microfluidic system that leverages isotachophoresis to fractionate and isolate cytoplasmic RNA and genomic DNA (gDNA) from single cells. The system uniquely enables independent, sequence-specific analyses of these critical markers. Our system uses a microfluidic chip with a simple geometry and four end-channel electrodes, and completes the entire process in <5 min, including lysis, purification, fractionation, and delivery to DNA and RNA output reservoirs, each containing high quality and purity aliquots with no measurable cross-contamination of cytoplasmic RNA versus gDNA. We demonstrate our system with simultaneous, sequence-specific quantitation using off-chip RT-qPCR and qPCR for simultaneous cytoplasmic RNA and gDNA analyses, respectively.
View details for DOI 10.1002/elps.201500040
View details for Web of Science ID 000358010400016
View details for PubMedID 25820552
-
Transient delivery of modified mRNA encoding TERT rapidly extends telomeres in human cells
FASEB JOURNAL
2015; 29 (5): 1930-1939
Abstract
Telomere extension has been proposed as a means to improve cell culture and tissue engineering and to treat disease. However, telomere extension by nonviral, nonintegrating methods remains inefficient. Here we report that delivery of modified mRNA encoding TERT to human fibroblasts and myoblasts increases telomerase activity transiently (24-48 h) and rapidly extends telomeres, after which telomeres resume shortening. Three successive transfections over a 4 d period extended telomeres up to 0.9 kb in a cell type-specific manner in fibroblasts and myoblasts and conferred an additional 28 ± 1.5 and 3.4 ± 0.4 population doublings (PD), respectively. Proliferative capacity increased in a dose-dependent manner. The second and third transfections had less effect on proliferative capacity than the first, revealing a refractory period. However, the refractory period was transient as a later fourth transfection increased fibroblast proliferative capacity by an additional 15.2 ± 1.1 PD, similar to the first transfection. Overall, these treatments led to an increase in absolute cell number of more than 10(12)-fold. Notably, unlike immortalized cells, all treated cell populations eventually stopped increasing in number and expressed senescence markers to the same extent as untreated cells. This rapid method of extending telomeres and increasing cell proliferative capacity without risk of insertional mutagenesis should have broad utility in disease modeling, drug screening, and regenerative medicine.-Ramunas, J., Yakubov, E., Brady, J. J., Corbel, S. Y., Holbrook, C., Brandt, M., Stein, J., Santiago, J. G., Cooke, J. P., Blau, H. M. Transient delivery of modified mRNA encoding TERT rapidly extends telomeres in human cells.
View details for DOI 10.1096/fj.14-259531
View details for Web of Science ID 000354114600027
-
Increasing Hybridization Rate and Sensitivity of Bead-Based Assays Using Isotachophoresis
ANGEWANDTE CHEMIE-INTERNATIONAL EDITION
2014; 53 (50): 13813-13816
Abstract
We present an electrokinetic technique to increase the reaction rate and sensitivity of bead-based assays. We use isotachophoresis (ITP) to preconcentrate and co-focus target molecules and beads into a single ITP zone. The process achieves rapid mixing, stirring, and strongly increases the binding reaction rate. We demonstrate our assay with quantitative detection of 24 nt single-stranded DNA over a dynamic range of three orders of magnitude and multiplexed detection of ten target species per sample. We show that ITP can achieve approximately the same sensitivity as a well-stirred standard reaction in 60-fold reduced reaction time (20 min versus 20 h). Alternately, compared to standard reaction times of 30 min, we show that 20 min ITP hybridization can achieve 5.3-fold higher sensitivity.
View details for DOI 10.1002/anie.201408403
View details for Web of Science ID 000345833100030
View details for PubMedID 25303671
-
Increasing hybridization rate and sensitivity of DNA microarrays using isotachophoresis
LAB ON A CHIP
2014; 14 (16): 2958-2967
Abstract
We present an on-chip electrokinetic method to increase the reaction kinetics and sensitivity of DNA microarray hybridization. We use isotachophoresis (ITP) to preconcentrate target molecules in solution and transport them over the immobilized probe sites of a microarray, greatly increasing the binding reaction rate. We show theoretically and experimentally that ITP-enhanced microarrays can be hybridized much faster and with higher sensitivity than conventional methods. We demonstrate our assay using a microfluidic system consisting of a PDMS microchannel superstructure bonded onto a glass slide on which 60 spots of 20-27 nt ssDNA oligonucleotide probes are immobilized. Our 30 min assay results in an 8.2 fold higher signal than the conventional overnight hybridization at 100 fM target concentration. We show rapid and quantitative detection over 4 orders of magnitude dynamic range of target concentration with no increase in the nonspecific signal. Our technique can be further multiplexed for higher density microarrays and extended for other reactions of target-surface immobilized ligands.
View details for DOI 10.1039/c4lc00374h
View details for Web of Science ID 000339470400010
View details for PubMedID 24921466
-
Simultaneous Purification and Fractionation of Nucleic Acids and Proteins from Complex Samples Using Bidirectional Isotachophoresis
ANALYTICAL CHEMISTRY
2014; 86 (15): 7264-7268
Abstract
We report on our efforts to create an on-chip system to simultaneously purify and fractionate nucleic acids and proteins from complex samples using isotachophoresis (ITP). We have developed this technique to simultaneously extract extracellular DNA and proteins from human blood serum samples and deliver these to two separate output reservoirs on a chip. The purified DNA is compatible with quantitative polymerase chain reaction (qPCR), and proteins can be extracted so as to exclude albumin, the most abundant protein in serum. We describe significant remaining challenges in making this bidirectional method a robust and efficient technique. These challenges include managing channel surface adsorption of proteins, identifying the cause of observed reductions in low molecular weight proteins, and dealing with nonspecific binding of proteins and DNA.
View details for DOI 10.1021/ac501299a
View details for Web of Science ID 000340081100019
-
Coupling Isotachophoresis with Affinity Chromatography for Rapid and Selective Purification with High Column Utilization, Part 2: Experimental Study
ANALYTICAL CHEMISTRY
2014; 86 (13): 6229-6236
View details for DOI 10.1021/ac5011074
View details for Web of Science ID 000338488800012
-
Coupling Isotachophoresis with Affinity Chromatography for Rapid and Selective Purification with High Column Utilization, Part 1: Theory
ANALYTICAL CHEMISTRY
2014; 86 (13): 6220-6228
View details for DOI 10.1021/ac5011052
View details for Web of Science ID 000338488800011
-
Purification of nucleic acids using isotachophoresis
JOURNAL OF CHROMATOGRAPHY A
2014; 1335: 105-120
Abstract
Reviewed are methods of nucleic acid (NA) extraction and sample preparation using an electrophoretic purification and focusing method called isotachophoresis (ITP). ITP requires no special surface chemistries or geometric structures, and can be achieved in a compact system with no moving parts. ITP is also compatible with a wide range of samples and lysing methods. Described are general principles of ITP, considerations around the application of ITP to biological samples (e.g., blood, urine and saliva), ITP electrolyte design considerations for fast and selective NA purification, and examples of ITP compatible lysing methods. Several of the challenges associated with purification of NAs are presented as well as methods to address these. Lastly, specific examples of lysing methods and ITP chemistries are described for purification of NA including host and pathogenic DNA, pathogenic rRNA, and host micro-RNA from complex sample matrices.
View details for DOI 10.1016/j.chroma.2013.12.027
View details for Web of Science ID 000334476200013
View details for PubMedID 24444800
-
An injection molded microchip for nucleic acid purification from 25 microliter samples using isotachophoresis
JOURNAL OF CHROMATOGRAPHY A
2014; 1331: 139-142
Abstract
We present a novel microchip device for purification of nucleic acids from 25μL biological samples using isotachophoresis (ITP). The device design incorporates a custom capillary barrier structure to facilitate robust sample loading. The chip uses a 2mm channel width and 0.15mm depth to reduce processing time, mitigate Joule heating, and achieve high extraction efficiency. To reduce pH changes in the device due to electrolysis, we incorporated a buffering reservoir physically separated from the sample output reservoir. To reduce dispersion of the ITP-focused zone, we used optimized turn geometries. The chip was fabricated by injection molding PMMA and COC plastics through a commercial microfluidic foundry. The extraction efficiency of nucleic acids from the device was measured using fluorescent quantification, and an average recovery efficiency of 81% was achieved for nucleic acid masses between 250pg and 250ng. The devices were also used to purify DNA from whole blood, and the extracted DNA was amplified using qPCR to show the PCR compatibility of the purified sample.
View details for DOI 10.1016/j.chroma.2014.01.036
View details for Web of Science ID 000332264900018
View details for PubMedID 24485540
-
On-Chip Separation and Analysis of RNA and DNA from Single Cells
ANALYTICAL CHEMISTRY
2014; 86 (4): 1953-1957
Abstract
The simultaneous analysis of RNA and DNA of single cells remains a challenge as these species have very similar physical and biochemical properties and can cross-contaminate each other. Presented is an on-chip system that enables selective lysing of single living cells, extraction, focusing, and absolute quantification of cytoplasmic RNA mass and its physical separation from DNA in the nucleus using electrical lysing and isotachophoresis (ITP). This absolute quantitation is performed without enzymatic amplification in less than 5 min. The nucleus is preserved, and its DNA fluorescence signal can be measured independently. We demonstrate the technique using single mouse lymphocyte cells, for which we extracted an average of 14.1 pg of total RNA per cell. We also demonstrate correlation analysis between the absolute amount of RNA and relative amount of DNA, showing heterogeneity associated with cell cycles. The technique is compatible with fractionation of DNA and RNA and with downstream assays of each.
View details for DOI 10.1021/ac4040218
View details for Web of Science ID 000331775600006
View details for PubMedID 24499009
-
In Situ Spatially and Temporally Resolved Measurements of Salt Concentration between Charging Porous Electrodes for Desalination by Capacitive Deionization
ENVIRONMENTAL SCIENCE & TECHNOLOGY
2014; 48 (3): 2008-2015
Abstract
Capacitive deionization (CDI) is an emerging water desalination technique. In CDI, pairs of porous electrode capacitors are electrically charged to remove salt from brackish water present between the electrodes. We here present a novel experimental technique allowing measurement of spatially and temporally resolved salt concentration between the CDI electrodes. Our technique measures the local fluorescence intensity of a neutrally charged fluorescent probe which is collisionally quenched by chloride ions. To our knowledge, our system is the first to measure in situ and spatially resolved chloride concentration in a laboratory CDI cell. We here demonstrate good agreement between our dynamic measurements of salt concentration in a charging, millimeter-scale CDI system to the results of a modified Donnan porous electrode transport model. Further, we utilize our dynamic measurements to demonstrate that salt removal between our charging CDI electrodes occurs on a longer time scale than the capacitive charging time scales of our CDI cell. Compared to typical measurements of CDI system performance (namely, measurements of outflow ionic conductivity), our technique can enable more advanced and better-controlled studies of ion transport in CDI systems, which can potentially catalyze future performance improvements.
View details for DOI 10.1021/es403682n
View details for Web of Science ID 000331015100078
View details for PubMedID 24433022
-
Particle Tracking and Multispectral Collocation Method for Particle-to-Particle Binding Assays
ANALYTICAL CHEMISTRY
2014; 86 (1): 608-614
Abstract
We present a simple-to-implement method for analyzing images of randomly distributed particles transported through a fluidic channel. We term this method particle imaging, tracking and collocation (PITC). Our method uses off-the-shelf optics including a CCD camera, epifluorescence microscope, and a dual-view color separator to image freely suspended particles in a wide variety of microchannels (with optical access for image collection). The particles can be transported via electrophoresis and/or pressure driven flow to increase throughput of analysis. We here describe the implementation of the algorithm and demonstrate and validate three of its capabilities: (1) identification of particle coordinates, (2) tracking of particle motion, and (3) monitoring of particle interaction via collocation analysis. We use Monte Carlo simulations for validation and optimization of the input parameters. We also present an experimental demonstration of the analysis on challenging image data, including a flow of two, interacting Brownian particle populations. In the latter example, we use PITC to detect the presence of target DNA by monitoring the hybridization-induced binding between the two populations of beads, each functionalized with DNA probes complementary to the target molecule.
View details for DOI 10.1021/ac402830q
View details for Web of Science ID 000329548700063
View details for PubMedID 24266609
-
Impedance-based study of capacitive porous carbon electrodes with hierarchical and bimodal porosity
JOURNAL OF POWER SOURCES
2013; 241: 266-273
View details for DOI 10.1016/j.jpowsour.2013.03.178
View details for Web of Science ID 000323093700034
-
Rapid High-Specificity microRNA Detection Using a Two-stage Isotachophoresis Assay
ANGEWANDTE CHEMIE-INTERNATIONAL EDITION
2013; 52 (44): 11534-11537
Abstract
Focusing in on the small: A two-stage microRNA detection assay uses electrokinetic focusing to speed up hybridization and a functionalized hydrogel for affinity purification. This method detects microRNAs in 15 minutes with single-nucleotide specificity, and processes only 5 ng of total RNA.
View details for DOI 10.1002/anie.201305875
View details for Web of Science ID 000330732700011
View details for PubMedID 24038732
-
Temperature Effects on Electrophoresis
ANALYTICAL CHEMISTRY
2013; 85 (10): 5103-5113
Abstract
We present a model capturing the important contributors to the effects of temperature on the observable electrophoretic mobilities of small ions, and on solution conductivity and pH. Our temperature model includes relations for temperature-dependent viscosity, ionic strength corrections, degree of ionization (pK), and ion solvation effects on mobility. We incorporate thermophysical data for water viscosity, temperature-dependence of the Onsager-Fuoss model for finite ionic strength effects on mobility, temperature-dependence of the extended Debye-Huckel theory for correction of ionic activity, the Clarke-Glew approach and tabulated thermodynamic quantities of ionization reaction for acid dissociation constants as a function of temperature, and species-specific, empirically evaluated correction terms for temperature-dependence of Stokes' radii. We incorporated our model into a MATLAB-based simulation tool we named Simulation of Temperature Effects on ElectroPhoresis (STEEP). We validated our model using conductivity and pH measurements across a temperature variation of 25-70 °C for a set of electrolytes routinely used in electrophoresis. The model accurately captures electrolyte solution pH and conductivity, including important effects not captured by simple Walden-type relations.
View details for DOI 10.1021/ac400447k
View details for Web of Science ID 000319651100038
View details for PubMedID 23627294
-
A method for non-invasive full-field imaging and quantification of chemical species.
Lab on a chip
2013; 13 (8): 1632-1643
Abstract
We present a novel method for full-field scalar visualization and quantification of species concentration fields. We term this method species-altered fluorescence imaging (SAFI). The method employs electrically neutral fluorescent dyes whose quantum yields are selectively quenched or enhanced by species of interest. SAFI enables simultaneous imaging of material interfaces and provides non-invasive, scalar-field quantitation of two-dimensional species concentration fields. We describe criteria for choosing SAFI dyes and tabulate 35 promising SAFI dyes and their relevant properties. Next, we describe species concentration quantification with SAFI via Stern-Volmer quenching and discuss the sensitivity and resolution of our method. We demonstrate this method with two dyes, 6-methoxy-N-(3-sulfopropyl)quinolinium (SPQ) and 10-(3-sulfopropyl)acridinium betaine (SAB). We demonstrate our method in full-field visualization of several challenging electrokinetic flows: isotachophoresis (ITP) in both cationic and anionic modes, and in a convective electrokinetic instability (EKI) flow. Through these experiments we collectively quantify ion concentration shock velocities, simultaneously measure concentrations of five species, and quantify the development of an unsteady, chaotic, 2D flow.
View details for DOI 10.1039/c3lc41293h
View details for PubMedID 23463253
-
Two- and three-dimensional modeling and optimization applied to the design of a fast hydrodynamic focusing microfluidic mixer for protein folding
PHYSICS OF FLUIDS
2013; 25 (3)
View details for DOI 10.1063/1.4793612
View details for Web of Science ID 000316951900006
-
Isotachophoresis with ionic spacer and two-stage separation for high sensitivity DNA hybridization assay
ANALYST
2013; 138 (11): 3117-3120
Abstract
We present an on-chip electrophoretic assay for rapid and high sensitivity nucleic acid (NA) detection. The assay uses isotachophoresis (ITP) to enhance NA hybridization and an ionic spacer molecule to subsequently separate reaction products. In the first stage, the probe and target focus and mix rapidly in free solution under ITP. The reaction mixture then enters a region containing a sieving matrix, which allows the spacer ion to overtake and separate the slower probe-target complex from free, unhybridized probes. This results in the formation of two focused ITP peaks corresponding to probe and probe-target complex signals. For a 149 nt DNA target, we achieve a 220 fM limit of detection (LOD) within 10 min, with a 3.5 decade dynamic range. This LOD constitutes a 12× improvement over previous ITP-based hybridization assays. The technique offers an alternative to traditional DNA hybridization assays, and can be multiplexed and extended to detect other biomolecules.
View details for DOI 10.1039/c3an00374d
View details for Web of Science ID 000318513500003
-
A method for non-invasive full-field imaging and quantification of chemical species
LAB ON A CHIP
2013; 13 (8): 1632-1643
View details for DOI 10.1039/c3lc41293h
View details for Web of Science ID 000316275200026
- Particle Tracking and Multispectral Collocation Method for Cytometry-Like and Particle-to-Particle Binding Assays Particle Tracking and Multispectral Collocation Method for Particle-to-Particle Binding Assays, Analytical Chemistry 2013; 1 (86): 608-614
-
Integration of rapid DNA hybridization and capillary zone electrophoresis using bidirectional isotachophoresis
ANALYST
2013; 138 (1): 87-90
Abstract
We present a method for rapid, sequence-specific detection of multiple DNA fragments by integrating isotachophoresis (ITP) based DNA hybridization and capillary zone electrophoresis (CZE) using bidirectional ITP. Our method leverages the high preconcentration ability of ITP to accelerate slow, second-order DNA hybridization kinetics, and the high resolving power of CZE to separate and identify reaction products. We demonstrate the speed and sensitivity of our assay by detecting 5 pM, 39 nt ssDNA target within 3 min, using a molecular beacon probe. We also demonstrate the feasibility of our assay for multiplexed detection of multiple-length ssDNA targets by simultaneously detecting 39 and 90 nt ssDNA targets.
View details for DOI 10.1039/c2an36249j
View details for Web of Science ID 000311823200007
-
Unraveling the potential and pore-size dependent capacitance of slit-shaped graphitic carbon pores in aqueous electrolytes
PHYSICAL CHEMISTRY CHEMICAL PHYSICS
2013; 15 (7): 2309-2320
Abstract
Understanding and leveraging physicochemical processes at the pore scale are believed to be essential to future performance improvements of supercapacitors and capacitive desalination (CD) cells. Here, we report on a combination of electrochemical experiments and fully atomistic simulations to study the effect of pore size and surface charge density on the capacitance of graphitic nanoporous carbon electrodes. Specifically, we used cyclic voltammetry (CV) and electrochemical impedance spectroscopy (EIS) to study the effect of potential and pore size on the capacitance of nanoporous carbon foams. Molecular dynamics simulations were performed to study the pore-size dependent accumulation of aqueous electrolytes in slit-shaped graphitic carbon pores of different widths (0.65 to 1.6 nm). Experimentally, we observe a pronounced increase of the capacitance of sub-nm pores as the applied potential window gets wider, from a few F g(-1) for narrow potential ranges (-0.3 to 0.3 V vs. Ag/AgCl) to ~40 F g(-1) for wider potential windows (-0.9 V to 0.9 V vs. Ag/AgCl). By contrast, the capacitance of wider pores does not depend significantly on the applied potential window. Molecular dynamics simulations confirm that the penetration of ions into pores becomes more difficult with decreasing pore width and increasing strength of the hydration shell. Consistent with our experimental results, we observe a pore- and ion-size dependent threshold-like charging behavior when the pore width becomes comparable to the size of the hydrated ion (0.65 nm pores for Na(+) and 0.79 nm pores for Cl(-) ions). The observed pore-size and potential dependent accumulation of ions in slit-shaped carbon pores can be explained by the hydration structure of the ions entering the charged pores. The results are discussed in view of their effect on energy-storage and desalination efficiency.
View details for DOI 10.1039/c2cp43361c
View details for Web of Science ID 000313891400008
View details for PubMedID 23295944
-
Coupling isotachophoresis and capillary electrophoresis: a review and comparison of methods
ANALYST
2013; 138 (3): 735-754
Abstract
We present a comprehensive review and comparison of the methodologies for increasing sensitivity and resolution of capillary electrophoresis (CE) using online transient isotachophoresis (tITP). We categorize the diverse set of coupled tITP and CE (tITP-CE) methods based on their fundamental principles for disrupting isotachophoretic preconcentration and triggering electrophoretic separation. Based on this classification, we discuss important features, advantages, limitations, and optimization principles of various tITP-CE methods. We substantiate our discussion with original simulations, instructive examples, and published experimental results.
View details for DOI 10.1039/c2an36150g
View details for Web of Science ID 000312944400002
View details for PubMedID 23232502
-
Integrated Printed Circuit Board Device for Cell Lysis and Nucleic Acid Extraction
ANALYTICAL CHEMISTRY
2012; 84 (21): 9640-9645
Abstract
Preparation of raw, untreated biological samples remains a major challenge in microfluidics. We present a novel microfluidic device based on the integration of printed circuit boards and an isotachophoresis assay for sample preparation of nucleic acids from biological samples. The device has integrated resistive heaters and temperature sensors as well as a 70 ?m × 300 ?m × 3.7 cm microfluidic channel connecting two 15 ?L reservoirs. We demonstrated this device by extracting pathogenic nucleic acids from 1 ?L dispensed volume of whole blood spiked with Plasmodium falciparum. We dispensed whole blood directly onto an on-chip reservoir, and the system's integrated heaters simultaneously lysed and mixed the sample. We used isotachophoresis to extract the nucleic acids into a secondary buffer via isotachophoresis. We analyzed the convective mixing action with micro particle image velocimetry (micro-PIV) and verified the purity and amount of extracted nucleic acids using off-chip quantitative polymerase chain reaction (PCR). We achieved a clinically relevant limit of detection of 500 parasites per microliter. The system has no moving parts, and the process is potentially compatible with a wide range of on-chip hybridization or amplification assays.
View details for DOI 10.1021/ac302622v
View details for Web of Science ID 000310664600107
View details for PubMedID 23046297
-
Effect of PVP on the electroosmotic mobility of wet-etched glass microchannels
ELECTROPHORESIS
2012; 33 (21): 3259-3262
Abstract
We present an experimental study on the effect of polymer PVP on EOF mobility of microchannels wet etched into optical white soda lime glass, also known as Crown glass. We performed experiments to evaluate the effect of PVP concentration and pH on EOF mobility. We used on-chip capillary zone electrophoresis and a neutral fluorescent dye as a passive marker to quantify the electroosmotic flow. We performed experiments under controlled conditions by varying pH from 5.2 and 10.3 and concentration of PVP from 0 to 2.0% w/w at constant ionic strength (30 mM). Our experiments show that PVP at concentrations of 1.0% or above very effectively suppress EOF at low pH (6.6). At high pH of 10.3, PVP has a much weaker suppressing effect on EOF and increasing its concentration above about 0.5% showed negligible effect on EOF mobility. Finally, we briefly discuss the effects of pH on using PVP as an adsorbed coating. Our experiments provide useful guidelines on choosing correct pH and concentration of PVP for effective EOF suppression in glass channels.
View details for DOI 10.1002/elps.201200336
View details for Web of Science ID 000310476600019
View details for PubMedID 23065690
-
Capacitive desalination with flow-through electrodes
ENERGY & ENVIRONMENTAL SCIENCE
2012; 5 (11): 9511-9519
View details for DOI 10.1039/c2ee21498a
View details for Web of Science ID 000310006200035
-
Robust and high-resolution simulations of nonlinear electrokinetic processes in variable cross-section channels
ELECTROPHORESIS
2012; 33 (19-20): 3036-3051
Abstract
We present a model and an associated numerical scheme to simulate complex electrokinetic processes in channels with nonuniform cross-sectional area. We develop a quasi-1D model based on local cross-sectional area averaging of the equations describing unsteady, multispecies, electromigration-diffusion transport. Our approach uses techniques of lubrication theory to approximate electrokinetic flows in channels with arbitrary variations in cross-section; and we include chemical equilibrium calculations for weak electrolytes, Taylor-Aris type dispersion due of nonuniform bulk flow, and the effects of ionic strength on species mobility and on acid-base equilibrium constants. To solve the quasi-1D governing equations, we provide a dissipative finite volume scheme that adds numerical dissipation at selective locations to ensure both unconditional stability and high accuracy. We couple the numerical scheme with a novel adaptive grid refinement algorithm that further improves the accuracy of simulations by minimizing numerical dissipation. We benchmark our numerical scheme with existing numerical schemes by simulating nonlinear electrokinetic problems, including ITP and electromigration dispersion in CZE. Simulation results show that our approach yields fast, stable, and high-resolution solutions using an order of magnitude less grid points compared to the existing dissipative schemes. To highlight our model's capabilities, we demonstrate simulations that predict increase in detection sensitivity of ITP in converging cross-sectional area channels. We also show that our simulations of ITP in variable cross-sectional area channels have very good quantitative agreement with published experimental data.
View details for DOI 10.1002/elps.201200264
View details for Web of Science ID 000310289600013
View details for PubMedID 22996734
-
Electric fields yield chaos in microflows
PROCEEDINGS OF THE NATIONAL ACADEMY OF SCIENCES OF THE UNITED STATES OF AMERICA
2012; 109 (36): 14353-14356
Abstract
We present an investigation of chaotic dynamics of a low Reynolds number electrokinetic flow. Electrokinetic flows arise due to couplings of electric fields and electric double layers. In these flows, applied (steady) electric fields can couple with ionic conductivity gradients outside electric double layers to produce flow instabilities. The threshold of these instabilities is controlled by an electric Rayleigh number, Ra(e). As Ra(e) increases monotonically, we show here flow dynamics can transition from steady state to a time-dependent periodic state and then to an aperiodic, chaotic state. Interestingly, further monotonic increase of Ra(e) shows a transition back to a well-ordered state, followed by a second transition to a chaotic state. Temporal power spectra and time-delay phase maps of low dimensional attractors graphically depict the sequence between periodic and chaotic states. To our knowledge, this is a unique report of a low Reynolds number flow with such a sequence of periodic-to-aperiodic transitions. Also unique is a report of strange attractors triggered and sustained through electric fluid body forces.
View details for DOI 10.1073/pnas.1204920109
View details for Web of Science ID 000308912600021
View details for PubMedID 22908251
-
Integration of On-Chip Isotachophoresis and Functionalized Hydrogels for Enhanced-Sensitivity Nucleic Acid Detection
ANALYTICAL CHEMISTRY
2012; 84 (15): 6366-6369
Abstract
We introduce an on-chip electrokinetic assay to perform high-sensitivity nucleic acid (NA) detection. This assay integrates electrokinetic sample focusing using isotachophoresis (ITP) with a background signal-removal strategy that employs photopatterened, DNA-functionalized hydrogels. In this multistage assay, ITP first enhances hybridization kinetics between target NAs and end-labeled complementary reporters. After enhanced hybridization, migration through a DNA-functionalized hydrogel region removes excess reporters through affinity interactions. We demonstrate our assay on microRNAs, an important class of low-abundance biomarkers. The assay exhibits 4 orders of magnitude dynamic range, near 1 pM detection limits starting from less than 100 fg of microRNA, and high selectivity for mature microRNA sequences, all within a 10 min run time. This new microfluidic framework provides a unique quantitative assay for NA detection.
View details for DOI 10.1021/ac301586q
View details for Web of Science ID 000307159200019
View details for PubMedID 22803507
-
Bacterial RNA Extraction and Purification from Whole Human Blood Using Isotachophoresis
ANALYTICAL CHEMISTRY
2012; 84 (14): 5858-5863
Abstract
We demonstrate a novel assay for physicochemical extraction and isotachophoresis-based purification of 16S rRNA from whole human blood infected with Pseudomonas putida . This on-chip assay is unique in that the extraction can be automated using isotachophoresis in a simple device with no moving parts, it protects RNA from degradation when isolating from ribonuclease-rich matrices (such as blood), and produces a purified total nucleic acid sample that is compatible with enzymatic amplification assays. We show that the purified RNA is compatible with reverse transcription-quantitative polymerase chain reaction (RT-qPCR) and demonstrate a clinically relevant sensitivity of 0.03 bacteria per nanoliter using RT-qPCR.
View details for DOI 10.1021/ac301021d
View details for Web of Science ID 000306441200006
View details for PubMedID 22816776
-
Rapid hybridization of nucleic acids using isotachophoresis
PROCEEDINGS OF THE NATIONAL ACADEMY OF SCIENCES OF THE UNITED STATES OF AMERICA
2012; 109 (28): 11127-11132
Abstract
We use isotachophoresis (ITP) to control and increase the rate of nucleic acid hybridization reactions in free solution. We present a new physical model, validation experiments, and demonstrations of this assay. We studied the coupled physicochemical processes of preconcentration, mixing, and chemical reaction kinetics under ITP. Our experimentally validated model enables a closed form solution for ITP-aided reaction kinetics, and reveals a new characteristic time scale which correctly predicts order 10,000-fold speed-up of chemical reaction rate for order 100 pM reactants, and greater enhancement at lower concentrations. At 500 pM concentration, we measured a reaction time which is 14,000-fold lower than that predicted for standard second-order hybridization. The model and method are generally applicable to acceleration of reactions involving nucleic acids, and may be applicable to a wide range of reactions involving ionic reactants.
View details for DOI 10.1073/pnas.1205004109
View details for Web of Science ID 000306642100027
View details for PubMedID 22733732
-
Concentration cascade of leading electrolyte using bidirectional isotachophoresis
ELECTROPHORESIS
2012; 33 (6): 1048-1059
Abstract
We present a novel method of creating concentration cascade of leading electrolyte (LE) in isotachophoresis (ITP) by using bidirectional ITP. ITP establishes ion-concentration shock waves between high-mobility LE and low-mobility trailing electrolyte (TE) ions. In bidirectional ITP, we set up simultaneous shock waves between anions and cations such that these waves approach each other and interact. The shock interaction causes a sudden decrease in LE concentration ahead of the focused anions and a corresponding decrease in analyte zone concentrations. This readjustment of analyte zone concentrations is accompanied by a corresponding increase in their zone lengths, in accordance to conservation laws. The method generates in situ gradient in the LE concentration, and therefore can be achieved in a single, straight channel simply by establishing the initial electrolyte chemistry. We have developed an analytical model useful in designing the process for maximum sensitivity and estimating increase in sample zone length due to shock interaction. We also illustrate the technique and evaluate its effectiveness in increasing detection sensitivity using transient simulations of species transport equations. We validated the theoretical predictions using experimental visualizations of bidirectional ITP zones for various electrolyte chemistries. Lastly, we use our technique to demonstrate a factor of 20 increase in the sensitivity of ITP-based detection of 2,4,6-trichlorophenol.
View details for DOI 10.1002/elps.201100510
View details for Web of Science ID 000303155700020
View details for PubMedID 22528425
-
On-chip Isotachophoresis for Separation of Ions and Purification of Nucleic Acids
JOVE-JOURNAL OF VISUALIZED EXPERIMENTS
2012
View details for DOI 10.3791/3890
View details for Web of Science ID 000209222800048
-
On-chip isotachophoresis for separation of ions and purification of nucleic acids.
Journal of visualized experiments : JoVE
2012: e3890-?
Abstract
Electrokinetic techniques are a staple of microscale applications because of their unique ability to perform a variety of fluidic and electrophoretic processes in simple, compact systems with no moving parts. Isotachophoresis (ITP) is a simple and very robust electrokinetic technique that can achieve million-fold preconcentration and efficient separation and extraction based on ionic mobility. For example, we have demonstrated the application of ITP to separation and sensitive detection of unlabeled ionic molecules (e.g. toxins, DNA, rRNA, miRNA) with little or no sample preparation and to extraction and purification of nucleic acids from complex matrices including cell culture, urine, and blood. ITP achieves focusing and separation using an applied electric field and two buffers within a fluidic channel system. For anionic analytes, the leading electrolyte (LE) buffer is chosen such that its anions have higher effective electrophoretic mobility than the anions of the trailing electrolyte (TE) buffer (Effective mobility describes the observable drift velocity of an ion and takes into account the ionization state of the ion, as described in detail by Persat et al.). After establishing an interface between the TE and LE, an electric field is applied such that LE ions move away from the region occupied by TE ions. Sample ions of intermediate effective mobility race ahead of TE ions but cannot overtake LE ions, and so they focus at the LE-TE interface (hereafter called the "ITP interface"). Further, the TE and LE form regions of respectively low and high conductivity, which establish a steep electric field gradient at the ITP interface. This field gradient preconcentrates sample species as they focus. Proper choice of TE and LE results in focusing and purification of target species from other non-focused species and, eventually, separation and segregation of sample species. We here review the physical principles underlying ITP and discuss two standard modes of operation: "peak" and "plateau" modes. In peak mode, relatively dilute sample ions focus together within overlapping narrow peaks at the ITP interface. In plateau mode, more abundant sample ions reach a steady-state concentration and segregate into adjoining plateau-like zones ordered by their effective mobility. Peak and plateau modes arise out of the same underlying physics, but represent distinct regimes differentiated by the initial analyte concentration and/or the amount of time allotted for sample accumulation. We first describe in detail a model peak mode experiment and then demonstrate a peak mode assay for the extraction of nucleic acids from E. coli cell culture. We conclude by presenting a plateau mode assay, where we use a non-focusing tracer (NFT) species to visualize the separation and perform quantitation of amino acids.
View details for DOI 10.3791/3890
View details for PubMedID 22415002
-
Desalination and hydrogen, chlorine, and sodium hydroxide production via electrophoretic ion exchange and precipitation
PHYSICAL CHEMISTRY CHEMICAL PHYSICS
2012; 14 (32): 11534-11545
Abstract
We demonstrate and analyze a novel desalination method which works by electrophoretically replacing sodium and chloride in feed salt water with a pair of ions, calcium and carbonate, that react and precipitate out. The resulting calcium carbonate precipitate is benign to health, and can be filtered or settled out, yielding low ionic strength product water. The ion exchange and precipitation employs self-sharpening interfaces induced by movement of multiple ions in an electric field to prevent contamination of the product water. Simultaneously, the electrolysis associated with the electromigration produces hydrogen gas, chlorine gas, and sodium hydroxide. We conducted an experimental study of this method's basic efficacy to desalinate salt water from 100 to 600 mol m(-3) sodium chloride. We also present physicochemical models of the process, and analyze replacement reagents consumption, permeate recovery ratio, and energy consumption. We hypothesize that the precipitate can be recycled back to replacement reagents using the well-known, commercially implemented Solvay process. We show that the method's permeate recovery ratio is 58% to 46%, which is on par with that of reverse osmosis. We show that the method's energy consumption requirement over and above that necessary to generate electrolysis is 3 to 10 W h l(-1), which is on par with the energy consumed by state-of-the-art desalination methods. Furthermore, the method operates at ambient temperature and pressure, and uses no specialized membranes. The process may be feasible as a part of a desalination-co-generation facility: generating fresh water, hydrogen and chlorine gas, and sodium hydroxide.
View details for DOI 10.1039/c2cp42121f
View details for Web of Science ID 000306708300034
View details for PubMedID 22806549
- An Integrated Printed Circuit Board Device for Cell Lysis and Nucleic Acid Extraction Analytical Chemistry 2012; 21 (84): 9640-9645
-
Extraction of DNA from Malaria-Infected Erythrocytes Using Isotachophoresis
ANALYTICAL CHEMISTRY
2011; 83 (24): 9715-9718
Abstract
We demonstrate a technique for purification of nucleic acids from malaria parasites infecting human erythrocytes using isotachophoresis (ITP). We release nucleic acids from malaria-infected erythrocytes by lysing with heat and proteinase K for 10 min and immediately, thereafter, load sample onto a capillary device. We study the effect of temperature on lysis efficiency. We also implement pressure-driven counterflow during ITP extraction to extend focusing time and increase nucleic acid yield. We show that the purified genomic DNA samples are compatible with polymerase chain reaction (PCR) and demonstrate a clinically relevant limit of detection of 0.5 parasites per nanoliter using quantitative PCR.
View details for DOI 10.1021/ac202567j
View details for Web of Science ID 000297946900077
View details for PubMedID 22074444
-
Electrophoretic mobility measurements of fluorescent dyes using on-chip capillary electrophoresis
ELECTROPHORESIS
2011; 32 (22): 3286-3294
Abstract
We present an experimental study of the effect of pH, ionic strength, and concentrations of the electroosmotic flow (EOF)-suppressing polymer polyvinylpyrrolidone (PVP) on the electrophoretic mobilities of commonly used fluorescent dyes (fluorescein, Rhodamine 6G, and Alexa Fluor 488). We performed on-chip capillary zone electrophoresis experiments to directly quantify the effective electrophoretic mobility. We use Rhodamine B as a fluorescent neutral marker (to quantify EOF) and CCD detection. We also report relevant acid dissociation constants and analyte diffusivities based on our absolute estimate (as per Nernst-Einstein diffusion). We perform well-controlled experiments in a pH range of 3-11 and ionic strengths ranging from 30 to 90? mM. We account for the influence of ionic strength on the electrophoretic transport of sample analytes through the Onsager and Fuoss theory extended for finite radii ions to obtain the absolute mobility of the fluorophores. Lastly, we briefly explore the effect of PVP on adsorption-desorption dynamics of all three analytes, with particular attention to cationic R6G.
View details for DOI 10.1002/elps.201100210
View details for Web of Science ID 000298098700026
View details for PubMedID 22102501
-
Coupled Isotachophoretic Preconcentration and Electrophoretic Separation Using Bidirectional Isotachophoresis
ANALYTICAL CHEMISTRY
2011; 83 (16): 6154-6162
Abstract
We present a novel technique for coupling isotachophoretic preconcentration and electrophoretic separation using bidirectional isotachophoresis (ITP). Bidirectional ITP simultaneously sets up sharp ITP interfaces between relatively high- and low-mobility cations and high- and low-mobility anions. These two interfaces can migrate toward each other and be described as ion concentration shock waves. We here demonstrate a bidirectional ITP process in which we use the interaction of these anionic and cationic ITP shock waves to trigger a transformation from ITP preconcentration to electrophoretic separation. We use anionic ITP to focus anionic sample species prior to shock interaction. The interaction of the counter-propagating anionic and cationic ITP shocks then changes the local pH (and ionic strength) of the focused analyte zones. Under this new condition, the analytes no longer focus and begin to separate electrophoretically. The method provides faster and much less dispersive transition from ITP preconcentration to electrophoretic separation compared with traditional (unidirectional) transient ITP. It eliminates the need for intermediate steps between focusing and separation, such as manual buffer exchanges. We illustrate the technique with numerical simulations of species transport equations. We have validated our simulations with experimental visualization of bidirectional ITP zones. We then show the effectiveness of the technique by coupling ITP preconcentration and high-resolution separation of a 1 kbp DNA ladder via shock interaction in bidirectional ITP.
View details for DOI 10.1021/ac200268f
View details for Web of Science ID 000293758800007
View details for PubMedID 21728346
-
Sample dispersion in isotachophoresis
JOURNAL OF FLUID MECHANICS
2011; 679: 455-475
View details for DOI 10.1017/jfm.2011.139
View details for Web of Science ID 000292644600018
-
Rapid Detection of Urinary Tract Infections Using Isotachophoresis and Molecular Beacons
ANALYTICAL CHEMISTRY
2011; 83 (11): 4110-4117
Abstract
We present a novel assay for rapid detection and identification of bacterial urinary tract infections using isotachophoresis (ITP) and molecular beacons. We applied on-chip ITP to extract and focus 16S rRNA directly from bacterial lysate and used molecular beacons to achieve detection of bacteria specific sequences. We demonstrated detection of E. coli in bacteria cultures as well as in patient urine samples in the clinically relevant range 1E6-1E8 cfu/mL. For bacterial cultures we further demonstrate quantification in this range. The assay requires minimal sample preparation (a single centrifugation and dilution), and can be completed, from beginning of lysing to detection, in under 15 min. We believe that the principles presented here can be used for design of other rapid diagnostics or detection methods for pathogenic diseases.
View details for DOI 10.1021/ac200253x
View details for Web of Science ID 000290978500022
View details for PubMedID 21545089
-
MicroRNA Profiling by Simultaneous Selective Isotachophoresis and Hybridization with Molecular Beacons
ANALYTICAL CHEMISTRY
2011; 83 (6): 2310-2316
Abstract
We present and demonstrate a novel assay for the detection and quantification of microRNA (miRNA) that leverages isotachophoresis (ITP) and molecular beacon (MB) hybridization. We use ITP to selectively preconcentrate miRNA from total RNA. We simultaneously focus MBs and use the ITP zone as a 10 pL reactor with active mixing where MBs fluoresce upon hybridization to target miRNA. To increase both sensitivity and selectivity, we leverage a multistage ITP strategy composed of three discrete regions of different concentrations of denaturant, sieving matrix, and magnesium chloride. We show that ITP hybridization is specific and selective to the miRNA target. We demonstrate ITP hybridization of miRNA in a biologically relevant case by detecting and quantifying miR-122 in human kidney and liver. ITP hybridization is a cheap, simple, high-speed, and amplification-free miRNA profiling method which requires small amounts (order 100 ng) of sample. The technique therefore represents an attractive alternative to PCR or Northern blot for miRNAs.
View details for DOI 10.1021/ac103225c
View details for Web of Science ID 000288182900060
View details for PubMedID 21329391
-
Electroosmotic pump performance is affected by concentration polarizations of both electrodes and pump
SENSORS AND ACTUATORS A-PHYSICAL
2011; 165 (2): 310-315
Abstract
Current methods of optimizing electroosmotic (EO) pump performance include reducing pore diameter and reducing ionic strength of the pumped electrolyte. However, these approaches each increase the fraction of total ionic current carried by diffuse electric double layer (EDL) counterions. When this fraction becomes significant, concentration polarization (CP) effects become important, and traditional EO pump models are no longer valid. We here report on the first simultaneous concentration field measurements, pH visualizations, flow rate, and voltage measurements on such systems. Together, these measurements elucidate key parameters affecting EO pump performance in the CP dominated regime. Concentration field visualizations show propagating CP enrichment and depletion fronts sourced by our pump substrate and traveling at order mm/min velocities through millimeter-scale channels connected serially to our pump. The observed propagation in millimeter-scale channels is not explained by current propagating CP models. Additionally, visualizations show that CP fronts are sourced by and propagate from the electrodes of our system, and then interact with the EO pump-generated CP zones. With pH visualizations, we directly detect that electrolyte properties vary sharply across the anode enrichment front interface. Our observations lead us to hypothesize possible mechanisms for the propagation of both pump- and electrode-sourced CP zones. Lastly, our experiments show the dynamics associated with the interaction of electrode and membrane CP fronts, and we describe the effect of these phenomena on EO pump flow rates and applied voltages under galvanostatic conditions.
View details for DOI 10.1016/j.sna.2010.10.002
View details for Web of Science ID 000288108500025
View details for PubMedID 21516230
-
High-sensitivity detection using isotachophoresis with variable cross-section geometry
ELECTROPHORESIS
2011; 32 (5): 563-572
Abstract
We present a theoretical and experimental study on increasing the sensitivity of ITP assays by varying channel cross-section. We present a simple, unsteady, diffusion-free model for plateau mode ITP in channels with axially varying cross-section. Our model takes into account detailed chemical equilibrium calculations and handles arbitrary variations in channel cross-section. We have validated our model with numerical simulations of a more comprehensive model of ITP. We show that using strongly convergent channels can lead to a large increase in sensitivity and simultaneous reduction in assay time, compared to uniform cross-section channels. We have validated our theoretical predictions with detailed experiments by varying channel geometry and analyte concentrations. We show the effectiveness of using strongly convergent channels by demonstrating indirect fluorescence detection with a sensitivity of 100 nM. We also present simple analytical relations for dependence of zone length and assay time on geometric parameters of strongly convergent channels. Our theoretical analysis and experimental validations provide useful guidelines on optimizing chip geometry for maximum sensitivity under constraints of required assay time, chip area and power supply.
View details for DOI 10.1002/elps.201000338
View details for Web of Science ID 000288094500010
View details for PubMedID 21308693
-
Toward an Electrolytic Micropump Actuator Design with Controlled Cyclic Bubble Growth and Recombination
SENSORS, ACTUATORS, AND MICROSYSTEMS (GENERAL) - 219TH ECS MEETING
2011; 35 (30): 3-11
View details for DOI 10.1149/1.3653918
View details for Web of Science ID 000300930300001
- High sensitivity detection using isotachophoresis with variable cross-section geometry Electrophoresis 2011; 32: 311-314
-
Quantification of Global MicroRNA Abundance by Selective Isotachophoresis
ANALYTICAL CHEMISTRY
2010; 82 (23): 9631-9635
Abstract
We here present and demonstrate a novel technique based on isotachophoresis (ITP) for the quantification of global microRNA (miRNA) abundance in total RNA. We leverage the selectivity of ITP to concentrate miRNA and exclude longer RNA molecules from the focused zone. We designed a novel ITP strategy where we initially establish three contiguous zones of sieving polymer, electrolyte, and denaturant concentrations. This allows for successive preconcentration, selection, and detection of miRNA. We optimized chemistry in each zone for high sensitivity and exquisite selectivity for miRNA. This technique allows for the measurement of the total miRNA content in a sample and its comparison between different cell types and tissues. We demonstrated and validated the efficacy of this technique by comparing global miRNA abundance in subconfluent and confluent cell cultures.
View details for DOI 10.1021/ac102496m
View details for Web of Science ID 000284668600009
View details for PubMedID 21062022
-
Design and fabrication of porous polymer wick structures
SENSORS AND ACTUATORS B-CHEMICAL
2010; 150 (2): 556-563
View details for DOI 10.1016/j.snb.2010.08.040
View details for Web of Science ID 000284339800010
-
A two-liquid electroosmotic pump using low applied voltage and power
SENSORS AND ACTUATORS A-PHYSICAL
2010; 163 (1): 311-314
View details for DOI 10.1016/j.sna.2010.07.008
View details for Web of Science ID 000283671000043
-
Active water management at the cathode of a planar air-breathing polymer electrolyte membrane fuel cell using an electroosmotic pump
JOURNAL OF POWER SOURCES
2010; 195 (11): 3640-3644
View details for DOI 10.1016/j.jpowsour.2009.12.025
View details for Web of Science ID 000275386100039
-
Passive water management at the cathode of a planar air-breathing proton exchange membrane fuel cell
JOURNAL OF POWER SOURCES
2010; 195 (10): 3201-3206
View details for DOI 10.1016/j.jpowsour.2009.12.030
View details for Web of Science ID 000275074200023
-
A self-priming, roller-free, miniature, peristaltic pump operable with a single, reciprocating actuator
SENSORS AND ACTUATORS A-PHYSICAL
2010; 160 (1-2): 141-146
View details for DOI 10.1016/j.sna.2010.04.018
View details for Web of Science ID 000279084100020
-
Effects of Constant Voltage on Time Evolution of Propagating Concentration Polarization
ANALYTICAL CHEMISTRY
2010; 82 (8): 3114-3117
Abstract
We extend the analytical theory of propagating concentration polarization (CP) to describe and compare the effects of constant-voltage versus constant-current conditions on the transient development of CP enrichment and depletion zones. We support our analysis with computational and experimental results. We find that at constant voltage, enrichment and depletion regions spread as t(1/2) as opposed to the previously observed t(1) scaling for constant current conditions. At low, constant voltages, the growth and propagation of CP zones can easily be misinterpreted as nonpropagating behavior.
View details for DOI 10.1021/ac100432q
View details for Web of Science ID 000276557600004
View details for PubMedID 20349992
-
In situ-polymerized wicks for passive water management in proton exchange membrane fuel cells
JOURNAL OF POWER SOURCES
2010; 195 (6): 1667-1675
View details for DOI 10.1016/j.jpowsour.2009.09.034
View details for Web of Science ID 000272580900020
-
Ionic strength effects on electrophoretic focusing and separations
ELECTROPHORESIS
2010; 31 (5): 910-919
Abstract
We present a numerical and experimental study of the effects of ionic strength on electrophoretic focusing and separations. We review the development of ionic strength models for electrophoretic mobility and chemical activity and highlight their differences in the context of electrophoretic separation and focusing simulations. We couple a fast numerical solver for electrophoretic transport with the Onsager-Fuoss model for actual ionic mobility and the extended Debye-Huckle theory for correction of ionic activity. Model predictions for fluorescein mobility as a function of ionic strength and pH compare well with data from CZE experiments. Simulation predictions of preconcentration factors in peak mode ITP also compare well with the published experimental data. We performed ITP experiments to study the effect of ionic strength on the simultaneous focusing and separation. Our comparisons of the latter data with simulation results at 10 and 250 mM ionic strength show the model is able to capture the observed qualitative differences in ITP analyte zone shape and order. Finally, we present simulations of CZE experiments where changes in the ionic strength result in significant change in selectivity and order of analyte peaks. Our simulations of ionic strength effects in capillary electrophoresis compare well with the published experimental data.
View details for DOI 10.1002/elps.200900560
View details for Web of Science ID 000275696400016
View details for PubMedID 20191554
-
Fluorescent Carrier Ampholytes Assay for Portable, Label-Free Detection of Chemical Toxins in Tap Water
ANALYTICAL CHEMISTRY
2010; 82 (5): 1858-1866
Abstract
We present a novel method for fluorescence-based indirect detection of analytes and demonstrate its use for label-free detection of chemical toxins in a hand-held device. We fluorescently label a mixture of low-concentration carrier ampholytes and introduce it into an isotachophoresis (ITP) separation. The carrier ampholytes provide a large number of fluorescent species with a wide range of closely spaced effective electrophoretic mobilities. Analytes focus under ITP and displace subsets of these carrier ampholytes. The analytes are detected indirectly and quantified by analyzing the gaps in the fluorescent ampholyte signal. The large number (on the order of 1000) of carrier ampholytes enables detection of a wide range of analytes, requiring little a priori knowledge of their electrophoretic properties. We discuss the principles of the technique and demonstrate its use in the detection of various analytes using a standard microscope system. We then present the integration of the technique into a self-contained hand-held device and demonstrate detection of chemical toxins (2-nitrophenol and 2,4,6-trichlorophenol) in tap water, with no sample preparation steps.
View details for DOI 10.1021/ac902526g
View details for Web of Science ID 000274841300044
View details for PubMedID 20141152
-
Method for Analyte Identification Using Isotachophoresis and a Fluorescent Carrier Ampholyte Assay
ANALYTICAL CHEMISTRY
2010; 82 (5): 2134-2138
Abstract
We present a novel method for identification of unlabeled analytes using fluorescent carrier ampholytes and isotachophoresis (ITP). The method is based on previous work where we showed that the ITP displacement of carrier ampholytes can be used for detection of unlabeled (nonfluorescent) analytes. We here propose a signal analysis method based on integration of the associated fluorescent signal. We define a normalized signal integral which is equivalent to an accurate measure of the amount of carrier ampholytes which are focused between the leading electrolyte and the analyte. We show that this parameter can be related directly to analyte effective mobility. Using several well characterized analytes, we construct calibration curves relating effective mobility and carrier ampholyte displacement at two different leading electrolyte (LE) buffers. On the basis of these calibration curves, we demonstrate the extraction of fully ionized mobility and dissociation constant of 2-nitrophenol and 2,4,6-trichlorophenol from ITP experiments with fluorescent carrier ampholytes. This extraction is based on no a priori assumptions or knowledge of these two toxic chemicals. This technique allows simultaneous identification of multiple analytes by their physiochemical properties in a few minutes and with no sample preparation.
View details for DOI 10.1021/ac9025658
View details for Web of Science ID 000274841300080
View details for PubMedID 20141174
-
Compact adaptive-grid scheme for high numerical resolution simulations of isotachophoresis
JOURNAL OF CHROMATOGRAPHY A
2010; 1217 (4): 588-599
Abstract
In a previous publication we demonstrated a fast simulation tool for solution of electrophoretic focusing and separation. We here describe the novel mathematical model and numerical algorithms used to create this code. These include the representation of advection-diffusion equations on an adaptive grid, high-resolution discretization of the equations (sixth order compact), a new variational-based approach for controlling the motion of grid points, and new boundary conditions which enable solution in a moving frame of reference. We discuss the advantages of combining a high-resolution discretization with an adaptive grid in accurately resolving sharp interfaces in isotachophoresis, and provide verification against known analytical solutions and comparison with prevailing exiting numerical algorithms.
View details for DOI 10.1016/j.chroma.2009.11.072
View details for Web of Science ID 000274479200020
View details for PubMedID 20022605
-
Evidence shows concentration polarization and its propagation can be key factors determining electroosmotic pump performance
SENSORS AND ACTUATORS B-CHEMICAL
2010; 143 (2): 795-798
View details for DOI 10.1016/j.snb.2009.10.005
View details for Web of Science ID 000274774100049
-
Theory and experiments of concentration polarization and ion focusing at microchannel and nanochannel interfaces
CHEMICAL SOCIETY REVIEWS
2010; 39 (3): 1014-1035
Abstract
In this tutorial review aimed at researchers using nanofluidic devices, we summarize the current state of theoretical and experimental approaches to describing concentration polarization (CP) in hybrid microfluidic-nanofluidic systems. We also analyze experimental results for these systems and place them in the context of recent theoretical developments. We then extend the theory to explain the behavior of both positively and negatively charged, low-concentration, analyte species in systems with CP. We conclude by discussing several applications of CP in microfluidics.
View details for DOI 10.1039/b902074h
View details for Web of Science ID 000274920300011
View details for PubMedID 20179822
-
Miniaturized system for isotachophoresis assays
LAB ON A CHIP
2010; 10 (17): 2242-2250
Abstract
We present an inexpensive hand-held device (240 g) that implements microchip isotachophoresis (ITP) with laser induced fluorescence (LIF) detection. This self-contained instrument integrates the functionality required for high voltage generation onto a microelectronic chip, includes LIF detection and is powered by a universal serial bus (USB) link connected to a laptop computer. Using this device we demonstrate focusing and detection of a fluorescent species with a limit of detection of 100 pM. We show that the response of the detector is linear with the initial analyte concentration, making this device suitable for quantitative analysis. We also demonstrate the use of our simulation tools for design and prediction of ITP assays, and validate these results with a demonstration of multiplexed indirect detection of (unlabeled) analytes performed using the device. We find good agreement between simulations and experimental results. Using a label-free isotachaphoresis assay implemented in the hand-held device we detect two explosives and an endocrine disruptor spiked in river water, with no prior sample processing.
View details for DOI 10.1039/c004120c
View details for Web of Science ID 000280812600010
View details for PubMedID 20571691
-
Purification of Nucleic Acids from Whole Blood Using Isotachophoresis
ANALYTICAL CHEMISTRY
2009; 81 (22): 9507-9511
Abstract
We present and demonstrate a novel technique for the purification of nucleic acids from biological samples using isotachophoresis (ITP). We demonstrate a simple and rapid method to achieve ITP-based extraction, preconcentration, and purification of DNA from nanoliter volumes of whole blood. We show that ITP purification yields genomic DNA samples which can be quantitated with fluorescence measurements and are immediately compatible with polymerase chain reaction (PCR) (e.g., a PCR-friendly solution free of significant inhibitors). We hypothesize ITP purification is applicable to processing of a wide range of complex biological samples.
View details for DOI 10.1021/ac901965v
View details for Web of Science ID 000271662400039
View details for PubMedID 19831356
-
Engineering model for coupling wicks and electroosmotic pumps with proton exchange membrane fuel cells for active water management
ELECTROCHIMICA ACTA
2009; 54 (26): 6223-6233
View details for DOI 10.1016/j.electacta.2009.05.001
View details for Web of Science ID 000270646600015
-
Two-phase hydrodynamics in a miniature direct methanol fuel cell
INTERNATIONAL JOURNAL OF HEAT AND MASS TRANSFER
2009; 52 (21-22): 5158-5166
View details for DOI 10.1016/j.ijheatmasstransfer.2009.05.003
View details for Web of Science ID 000270164200054
-
Electrokinetic control of sample splitting at a channel bifurcation using isotachophoresis
NEW JOURNAL OF PHYSICS
2009; 11
View details for DOI 10.1088/1367-2630/11/7/075026
View details for Web of Science ID 000268699200013
-
Effects of carbon dioxide on peak mode isotachophoresis: Simultaneous preconcentration and separation
LAB ON A CHIP
2009; 9 (10): 1377-1384
Abstract
We present a method that achieves simultaneous preconcentration and separation of analytes using peak-mode isotachophoresis with a single step injection in simple, off-the-shelf microchannels or capillaries. We leverage ions resulting from dissolved atmospheric carbon dioxide to weakly disrupt isotachophoretic preconcentration and induce separation of analyte species. We experimentally study the region between the leading and trailing electrolytes, and individually identify the carbonate and carbamate zones that result from the hydration and carbamation reaction of dissolved atmospheric carbon dioxide, respectively. The width of these zones and the gradient regions between them grow with time and create an electric field gradient that causes analytes to separate. Using this assay, we achieve focusing and separation of a 25 bp DNA ladder in a straight, 34 microm wide microchannel in a single loading step. As a demonstration of the fractionation capabilities of the assay, we show simultaneous preconcentration and separation of a DNA ladder from two proteins, GFP and allophycocyanin.
View details for DOI 10.1039/b815460k
View details for Web of Science ID 000268227400010
View details for PubMedID 19417904
-
Imaging and Quantification of Isotachophoresis Zones Using Nonfocusing Fluorescent Tracers
ANALYTICAL CHEMISTRY
2009; 81 (8): 3022-3028
Abstract
We present a novel method for visualizing isotachophoresis (ITP) zones. We introduce negligibly small concentrations of a fluorophore that is not focused by isotachophoresis. This nonfocusing tracer (NFT) migrates through multiple isotachophoresis zones. As it enters each zone, the NFT concentration adapts to the local electric field in each zone. ITP zones can then be visualized with a point detector or camera. The method can be used to detect, identify, and quantify unknown analyte zones and can visualize complex and even transient electrophoresis processes. This visualization technique is particularly suited to microfluidic and laboratory-on-a-chip applications, as typical fluorescence microscopes and charge-coupled device (CCD) cameras can provide high-resolution spatiotemporal data. We present a theoretical description, a methodology for identifying analytes, and experimental validation. We also visualize and analyze a complex, transient DNA ITP preconcentration and separation.
View details for DOI 10.1021/ac802698a
View details for Web of Science ID 000265158800025
View details for PubMedID 19290665
-
On the Propagation of Concentration Polarization from Microchannel-Nanochannel Interfaces Part II: Numerical and Experimental Study
LANGMUIR
2009; 25 (6): 3909-3916
Abstract
We present results of a combined computational and experimental study of the propagation of concentration polarization (CP) zones in a microchannel-nanochannel system. Our computational model considers the combined effects of bulk flow, electromigration, and diffusion and accurately captures the dynamics of CP. Using wall charge inside the nanochannel as a single fitting parameter, we predict experimentally observed enrichment and depletion shock velocities. Our model can also be used to compute the existence of CP with propagating enrichment and depletion shocks on the basis of measured ion mobility and wall properties. We present experiments where the background electrolyte consists of only a fluorescent ion and its counterion. These results are used to validate the computational model and to confirm predicted trends from an analytical model presented in the first of this two-paper series. We show experimentally that the enrichment region concentration is effectively independent of the applied current, while the enrichment and depletion shock velocities increase in proportion to current density.
View details for DOI 10.1021/1a803318e
View details for Web of Science ID 000264145000085
View details for PubMedID 19275188
-
On the Propagation of Concentration Polarization from Microchannel-Nanochannel Interfaces Part I: Analytical Model and Characteristic Analysis
LANGMUIR
2009; 25 (6): 3898-3908
Abstract
We develop two models to describe ion transport in variable-height micro- and nanochannels. For the first model, we obtain a one-dimensional (unsteady) partial differential equation governing flow and charge transport through a shallow and wide electrokinetic channel. In this model, the effects of electric double layer (EDL) on axial transport are taken into account using exact solutions of the Poisson-Boltzmann equation. The second simpler model, which is approachable analytically, assumes that the EDLs are confined to near-wall regions. Using a characteristics analysis, we show that the latter model captures concentration polarization (CP) effects and provides useful insight into its dynamics. Two distinct CP regimes are identified: CP with propagation in which enrichment and depletion shocks propagate outward, and CP without propagation where polarization effects stay local to micro- nanochannel interfaces. The existence of each regime is found to depend on a nanochannel Dukhin number and mobility of the co-ion nondimensionalized by electroosmotic mobility. Interestingly, microchannel dimensions and axial diffusion are found to play an insignificant role in determining whether CP propagates. The steady state condition of propagating CP is shown to be controlled by channel heights, surface chemistry, and co-ion mobility instead of the reservoir condition. Both models are validated against experimental results in Part II of this two-paper series.
View details for DOI 10.1021/1a803317p
View details for Web of Science ID 000264145000084
View details for PubMedID 19275187
-
Electrokinetics in nanochannels. Part II. Mobility dependence on ion density and ionic current measurements (vol 325, pg 539, 2008)
JOURNAL OF COLLOID AND INTERFACE SCIENCE
2009; 331 (2): 550-550
View details for DOI 10.1016/j.jcis.2008.12.019
View details for Web of Science ID 000263335700044
-
Electrokinetics in nanochannels. Part I. Electric double layer overlap and channel-to-well equilibrium (vol 325, pg 526, 2008)
JOURNAL OF COLLOID AND INTERFACE SCIENCE
2009; 331 (2): 549-549
View details for DOI 10.1016/j.jcis.2008.12.013
View details for Web of Science ID 000263335700043
-
Dry gas operation of proton exchange membrane fuel cells with parallel channels: Non-porous versus porous plates
JOURNAL OF POWER SOURCES
2009; 188 (1): 82-88
View details for DOI 10.1016/j.jpowsour.2008.11.069
View details for Web of Science ID 000264391400012
-
Open source simulation tool for electrophoretic stacking, focusing, and separation
JOURNAL OF CHROMATOGRAPHY A
2009; 1216 (6): 1008-1018
Abstract
We present the development, formulation, and performance of a new simulation tool for electrophoretic preconcentration and separation processes such as capillary electrophoresis, isotachophoresis, and field amplified sample stacking. The code solves the one-dimensional transient advection-diffusion equations for multiple multivalent weak electrolytes (including ampholytes) and includes a model for pressure-driven flow and Taylor-Aris dispersion. The code uses a new approach for the discretization of the equations, consisting of a high resolution compact scheme which is combined with an adaptive grid algorithm. We show that this combination allows for accurate resolution of sharp concentration gradients at high electric fields, while at the same time significantly reducing the computational time. We demonstrate smooth, stable, and accurate solutions at current densities as high as 5000A/m(2) using only 300 grid points, and a 75-fold reduction in computational time compared with equivalent uniform grid techniques. The code is available as an open source for free at http://microfluidics.stanford.edu.
View details for DOI 10.1016/j.chroma.2008.12.022
View details for Web of Science ID 000263087700017
View details for PubMedID 19124132
-
IN-SITU POLYMERIZED WICKS FOR PASSIVE WATER MANAGEMENT IN PEM FUEL CELL SYSTEMS
ES2009: PROCEEDINGS OF THE ASME 3RD INTERNATIONAL CONFERENCE ON ENERGY SUSTAINABILITY, VOL 1
2009: 325-326
View details for Web of Science ID 000281910700038
- Corrigendum to ‘Electrokinetics in Nanochannels: Part II: Mobility Dependence on Ion Density and Ionic Current Measurements Journal of Colloid and Interface Science 2009; 2 (331): 550-550
- Corrigendum to ‘Electrokinetics in Nanochannels. Part I: Electric Double Layer Overlap and Channel-to-Well Equilibrium Journal of Colloid and Interface Science 2009; 2 (331): 549-549
-
In-situ Polymerized Wicks for Passive Water Management and Humidification of Dry Gases
PROTON EXCHANGE MEMBRANE FUEL CELLS 9
2009; 25 (1): 303-309
View details for DOI 10.1149/1.3210581
View details for Web of Science ID 000329585500028
-
Special issue on fundamental principles and techniques in microfluidics
LAB ON A CHIP
2009; 9 (17): 2423-2424
View details for DOI 10.1039/b913538n
View details for Web of Science ID 000268975200001
View details for PubMedID 19680567
-
Basic principles of electrolyte chemistry for microfluidic electrokinetics. Part II: Coupling between ion mobility, electrolysis, and acid-base equilibria
LAB ON A CHIP
2009; 9 (17): 2454-2469
Abstract
We present elements of electrolyte dynamics and electrochemistry relevant to microfluidic electrokinetics experiments. In Part I of this two-paper series, we presented a review and introduction to the fundamentals of acid-base chemistry. Here, we first summarize the coupling between acid-base equilibrium chemistry and electrophoretic mobilities of electrolytes, at both infinite and finite dilution. We then discuss the effects of electrode reactions on microfluidic electrokinetic experiments and derive a model for pH changes in microchip reservoirs during typical direct-current electrokinetic experiments. We present a model for the potential drop in typical microchip electrophoresis device. The latter includes finite element simulation to estimate the relative effects of channel and reservoir dimensions. Finally, we summarize effects of electrode and electrolyte characteristics on potential drop in microfluidic devices. As a whole, the discussions highlight the importance of the coupling between electromigration and electrophoresis, acid-base equilibria, and electrochemical reactions.
View details for DOI 10.1039/b906468k
View details for Web of Science ID 000268975200004
View details for PubMedID 19680571
-
Hydrodynamic interactions in metal rodlike-particle suspensions due to induced charge electroosmosis
PHYSICAL REVIEW E
2009; 79 (1)
Abstract
We present a theoretical and experimental study of the role of hydrodynamic interactions on the motion and dispersion of metal rodlike particles in the presence of an externally applied electric field. In these systems, the electric field polarizes the particles and induces an electroosmotic flow relative to the surface of each particle. The simulations include the effect of the gravitational body force, buoyancy, far-field hydrodynamic interactions, and near-field lubrication forces. The particles in the simulations and experiments were observed to experience repeated pairing interactions in which they come together axially with their ends approaching each other, slide past one another until their centers approach, and then push apart. These interactions were confirmed in measurements of particle orientations and velocities, pair distribution functions, and net dispersion of the suspension. For large electric fields, the pair distribution functions show accumulation and depletion regions consistent with many pairing events. For particle concentrations of 10;{8}particles/mL and higher, dispersion within the suspension dramatically increases with increased field strength.
View details for DOI 10.1103/PhysRevE.79.011402
View details for Web of Science ID 000262976600043
View details for PubMedID 19257030
-
Rapid and selective extraction, isolation, preconcentration, and quantitation of small RNAs from cell lysate using on-chip isotachophoresis
LAB ON A CHIP
2009; 9 (15): 2145-2152
Abstract
We present a technique which enables the separation of small RNAs-such as microRNAs (miRNAs), short interfering RNAs (siRNAs), and Piwi-interacting RNAs (piRNAs)-from >or=66 nucleotide RNAs and other biomolecules contained in a cell lysate. In particular, the method achieves separation of small RNAs from precursor miRNAs (pre-miRNAs) in less than 3 min. We use on-chip isotachophoresis (ITP) for the simultaneous extraction, isolation, preconcentration and quantitation of small RNAs (approximately 22 nucleotides) and employ the high-efficiency sieving matrix Pluronic F-127; a thermo-responsive triblock copolymer which allows convenient microchannel loading at low temperature. We present the isolation of small RNAs from the lysate of 293A human kidney cells, and quantitate the number of short RNA molecules per cell to be 2.9x10(7). We estimate this quantity is an aggregate of roughly 500 types of short RNA molecules per 293A cell. Currently, the minimal cell number for small RNA extraction and detection with our method is approximately 900 (from a 5 microL sample volume), and we believe that small RNA analysis from tens of cells is realizable. Techniques for rapid and sensitive extraction and isolation of small RNAs from cell lysate are much-needed to further uncover their full range and functionality, including RNA interference studies.
View details for DOI 10.1039/b903542g
View details for Web of Science ID 000268033900005
View details for PubMedID 19606290
-
Basic principles of electrolyte chemistry for microfluidic electrokinetics. Part I: Acid-base equilibria and pH buffers
LAB ON A CHIP
2009; 9 (17): 2437-2453
Abstract
We review fundamental and applied acid-base equilibrium chemistry useful to microfluidic electrokinetics. We present elements of acid-base equilibrium reactions and derive rules for pH calculation for simple buffers. We also present a general formulation to calculate pH of more complex, arbitrary mixtures of electrolytes, and discuss the effects of ionic strength and temperature on pH calculation. More practically, we offer advice on buffer preparation and on buffer reporting. We also discuss "real world" buffers and likely contamination sources. In particular, we discuss the effects of atmospheric carbon dioxide on buffer systems, namely, the increase in ionic strength and acidification of typical electrokinetic device buffers. In Part II of this two-paper series, we discuss the coupling of acid-base equilibria with electrolyte dynamics and electrochemistry in typical microfluidic electrokinetic systems.
View details for DOI 10.1039/b906465f
View details for Web of Science ID 000268975200003
View details for PubMedID 19680570
-
NANOPORE CONCENTRATION POLARIZATION
PROCEEDINGS OF THE ASME INTERNATIONAL MECHANICAL ENGINEERING CONGRESS AND EXPOSITION, VOL 13, PTS A AND B
2009: 871-872
View details for Web of Science ID 000266546900113
-
Electrokinetics in nanochannels - Part I. Electric double layer overlap and channel-to-well equilibrium
JOURNAL OF COLLOID AND INTERFACE SCIENCE
2008; 325 (2): 526-538
Abstract
In this paper a new model is described for calculating the electric potential field in a long, thin nanochannel with overlapped electric double layers. Electrolyte concentration in the nanochannel is predicted self-consistently via equilibrium between ionic solution in the wells and within the nanochannel. Differently than published models that require detailed iterative numerical solutions of coupled differential equations, the framework presented here is self-consistent and predictions are obtained solving a simple one-dimensional integral. The derivation clearly shows that the electric potential field depends on three new parameters: the ratio of ion density in the channel to ion density in the wells; the ratio of free-charge density to bulk ion density within the channel; and a modified Debye-Hückel thickness, which is the relevant scale for shielding of surface net charge. For completeness, three wall-surface boundary conditions are analyzed: specified zeta-potential; specified surface net charge density; and charge regulation. Predictions of experimentally observable quantities based on the model proposed here, such as depth-averaged electroosmotic flow and net ionic current, are significantly different than results from previous overlapped electric double layer models. In this first paper of a series of two, predictions are presented where channel depth is varied at constant well concentration. Results show that under conditions of electric double layer overlap, electroosmosis contributes only a small fraction of the net ionic current, and that most of the measurable current is due to ionic conduction in conditions of increased counterion density in the nanochannel. In the second of this two-paper series, predictions are presented where well-concentration is varied and the channel depth is held constant, and the model described here is employed to study the dependence of ion mobility on ionic strength, and compare predictions to measurements of ionic current as a function of channel depth and ion density.
View details for DOI 10.1016/j.jcis.2008.06.007
View details for Web of Science ID 000258553900033
View details for PubMedID 18639883
-
Electrokinetics in nanochannels - Part II. Mobility dependence on ion density and ionic current measurements
JOURNAL OF COLLOID AND INTERFACE SCIENCE
2008; 325 (2): 539-546
Abstract
In the first of this two-paper series, a new model was developed for calculating the electric potential field in a long, thin nanochannel with overlapped electric double layers. The model takes into account the dependence of ion mobility on local ion densities and pH. This model is used here to study and demonstrate the effect of ion density and pH on ionic current measurements. A comparison is shown of predictions based on each of three boundary conditions, as studied in Part I. The model developed in Part I is validated by comparing simulations with measurements of ionic current as a function of sodium borate concentration. Results show that predictions based on extended Debye-Hückel theory for ion mobility significantly improve the accuracy of simulations, but that these do not predict exact scaling behavior. A simple bulk conductivity measurement used as input parameter for the simulations, in place of the predicted bulk conductivity (K(0)), guarantees agreement with data in the thin EDL region. Results also indicate that the charge regulation boundary condition, complemented with an adequate bulk electrolyte model, provides better agreement with experimental trends than the specified zeta potential or specified surface net charge boundary conditions. Further, it is shown that currents due to advection (by electroosmotic flow) are in all cases studied less than 25% of the total current in the system.
View details for DOI 10.1016/j.jcis.2008.06.008
View details for Web of Science ID 000258553900034
View details for PubMedID 18639884
-
Lymphocyte electrotaxis in vitro and in vivo
JOURNAL OF IMMUNOLOGY
2008; 181 (4): 2465-2471
Abstract
Electric fields are generated in vivo in a variety of physiologic and pathologic settings, including penetrating injury to epithelial barriers. An applied electric field with strength within the physiologic range can induce directional cell migration (i.e., electrotaxis) of epithelial cells, endothelial cells, fibroblasts, and neutrophils suggesting a potential role in cell positioning during wound healing. In the present study, we investigated the ability of lymphocytes to respond to applied direct current (DC) electric fields. Using a modified Transwell assay and a simple microfluidic device, we show that human PBLs migrate toward the cathode in physiologically relevant DC electric fields. Additionally, electrical stimulation activates intracellular kinase signaling pathways shared with chemotactic stimuli. Finally, video microscopic tracing of GFP-tagged immunocytes in the skin of mouse ears reveals that motile cutaneous T cells actively migrate toward the cathode of an applied DC electric field. Lymphocyte positioning within tissues can thus be manipulated by externally applied electric fields, and may be influenced by endogenous electrical potential gradients as well.
View details for Web of Science ID 000258345300026
View details for PubMedID 18684937
-
Sample zone dynamics in peak mode isotachophoresis
ANALYTICAL CHEMISTRY
2008; 80 (16): 6300-6307
Abstract
We present a theoretical and experimental study of analyte preconcentration via peak mode isotachophoresis (ITP). We perform perturbation analysis of the governing equations that includes electromigration, diffusion, buffer reactions, and nonlinear ionic strength effects. This analysis relaxes the inherent numerical stiffness and achieves a fast solution to the transient sample evolution problem. In this model, we have incorporated a semiempirical relation to capture dispersion phenomenon within ITP interfaces. We also present a simple, closed-form analytical model that identifies key parameters governing the preconcentration dynamics in peak mode ITP. We have validated our models through a detailed experimental study performed in constant current conditions. The relevant governing experiment parameters were varied independently; namely, the leading electrolyte concentration, trailing electrolyte concentration, and current. Through our experimental study, we have identified optimum conditions to achieve high preconcentration ratio and sample accumulation rates. Our approach to the theoretical problem and experimental study provides useful guidelines in optimizing parameters such as detector location, ITP duration, and electrolyte composition in ITP preconcentration and separation assays.
View details for DOI 10.1021/ac800792g
View details for Web of Science ID 000258448100021
View details for PubMedID 18642874
-
A depth-averaged electrokinetic flow model for shallow microchannels
JOURNAL OF FLUID MECHANICS
2008; 608: 43-70
View details for DOI 10.1017/S0022112008001869
View details for Web of Science ID 000258201900003
-
Ballistic dispersion in temperature gradient focusing
PROCEEDINGS OF THE ROYAL SOCIETY A-MATHEMATICAL PHYSICAL AND ENGINEERING SCIENCES
2008; 464 (2091): 595-612
View details for DOI 10.1098/rspa.2007.0161
View details for Web of Science ID 000252763200005
-
High flow rate per power electroosmotic pumping using low ion density solvents
SENSORS AND ACTUATORS A-PHYSICAL
2008; 141 (1): 201-212
View details for DOI 10.1016/j.sna.2007.07.023
View details for Web of Science ID 000253390400027
-
On-chip preconcentration and separation of simple and complex analytes using isotachophoresis
INTERNATIONAL MECHANICAL ENGINEERING CONGRESS AND EXPOSITION 2007, VOL 11 PT A AND PT B: MICRO AND NANO SYSTEMS
2008: 857-861
View details for Web of Science ID 000254834900111
- Taylor Dispersion in Sample Pre-Concentration Methods CRC Handbook of Electrophoresis edited by Landers, J. CRC Press. 2008; 3rd: 1085-1120
-
INDIRECT FLUORESCENCE DETECTION OF NON FLUORESCENT ANALYTES USING ISOTACHOPHORETIC MOBILITY MARKERS
PROCEEDINGS OF THE 6TH INTERNATIONAL CONFERENCE ON NANOCHANNELS, MICROCHANNELS, AND MINICHANNELS, PTS A AND B
2008: 1701-1706
View details for Web of Science ID 000262925200215
-
On-chip indirect detection of non-fluorescent analytes using fluorescent spacers
INTERNATIONAL MECHANICAL ENGINEERING CONGRESS AND EXPOSITION 2007, VOL 11 PT A AND PT B: MICRO AND NANO SYSTEMS
2008: 901-904
View details for Web of Science ID 000254834900118
-
Two-liquid electroosmotic pump for portable drug delivery systems
INTERNATIONAL MECHANICAL ENGINEERING CONGRESS AND EXPOSITION 2007, VOL 11 PT A AND PT B: MICRO AND NANO SYSTEMS
2008: 963-964
View details for Web of Science ID 000254834900128
-
Preconcentration, separation, and indirect detection of nonfluorescent analytes using fluorescent mobility markers
ANALYTICAL CHEMISTRY
2008; 80 (1): 279-286
Abstract
We present a method to achieve separation and indirect detection of nonfluorescent species using fluorescent mobility markers. This technique leverages isotachophoresis (ITP) for both preconcentration and separation. We employ a leading electrolyte (LE), trailing electrolyte (TE), and a set of fluorescent markers of mobilities designed to bound those of nonfluorescent analytes of interest. Fluorescent markers and nonfluorescent analytes are initially mixed homogenously and ITP is initiated. The dynamics of isotachophoresis cause the analyte and fluorescent marker mixture to segregate into respective zones between the LE and TE in the order of reducing mobility. Unlabeled analytes are detected as gaps (regions with local minimums in intensity) in the fluorescent signals of mobility markers. We have successfully demonstrated preconcentration, separation, and detection of unlabeled amino acids serine, glycine, and phenylalanine; and of acetic acid, aspartic acid, and 3-phenylpropionic acid. We show detection of 12 microM concentration of analytes with signal-to-noise ratio of 4.0 and with a high degree of repeatability. We discuss methods for encoding mobility marker identity using marker fluorescence intensity level and alternating fluorescence emission wavelengths. We present example experimental results of fluorescence intensity level encoding.
View details for DOI 10.1021/ac701706h
View details for Web of Science ID 000252026900042
View details for PubMedID 18031059
- Quick Measurement of Electroosmotic Flow Velocity Chips & Tips, Lab on a Chip 2008
-
Physics of pumping methanol/water solutions for fuel cell applications
PROCEEDINGS OF THE ASME INTERNATIONAL MECHANICAL ENGINEERING CONGRESS AND EXPOSITION 2007, VOL 6
2008: 637-642
View details for Web of Science ID 000254474800072
-
Model and Experimental Study of Hydrodynamic Coupling between a Fuel Pump and a Direct Methanol Fuel Cell
PROTON EXCHANGE MEMBRANE FUEL CELLS 8, PTS 1 AND 2
2008; 16 (2): 1525-1538
View details for DOI 10.1149/1.2981993
View details for Web of Science ID 000271859300156
-
On-chip isothermal polymerase chain reaction
INTERNATIONAL MECHANICAL ENGINEERING CONGRESS AND EXPOSITION 2007, VOL 11 PT A AND PT B: MICRO AND NANO SYSTEMS
2008: 1003-1004
View details for Web of Science ID 000254834900134
-
Experimental study of concentration polarization at a microchannel-nanochannel interface
INTERNATIONAL MECHANICAL ENGINEERING CONGRESS AND EXPOSITION 2007, VOL 11 PT A AND PT B: MICRO AND NANO SYSTEMS
2008: 911-912
View details for Web of Science ID 000254834900120
-
Toward orientation-independent design for gas recombination in closed-loop electroosmotic pumps
SENSORS AND ACTUATORS B-CHEMICAL
2007; 128 (1): 334-339
View details for DOI 10.1016/j.snb.2007.05.029
View details for Web of Science ID 000251465000046
-
Investigation of internal pressure gradients generated in electrokinetic flows with axial conductivity gradients
EXPERIMENTS IN FLUIDS
2007; 43 (6): 959-967
View details for DOI 10.1007/s00348-007-0366-3
View details for Web of Science ID 000251010400011
-
Free-surface microfluidic control of surface-enhanced Raman spectroscopy for the optimized detection of airborne molecules
PROCEEDINGS OF THE NATIONAL ACADEMY OF SCIENCES OF THE UNITED STATES OF AMERICA
2007; 104 (48): 18898-18901
Abstract
We present a microfluidic technique for sensitive, real-time, optimized detection of airborne water-soluble molecules by surface-enhanced Raman spectroscopy (SERS). The method is based on a free-surface fluidic device in which a pressure-driven liquid microchannel flow is constrained by surface tension. A colloidal suspension of silver nanoparticles flowing through the microchannel that is open to the atmosphere absorbs gas-phase 4-aminobenzenethiol (4-ABT) from the surrounding environment. As surface ions adsorbed on the colloid nanoparticles are substituted by 4-ABT, the colloid aggregates, forming SERS "hot spots" whose concentrations vary predictably along the microchannel flow. 4-ABT confined in these hot spots produces SERS spectra of very great intensity. An aggregation model is used to account quantitatively for the extent of colloid aggregation as determined from the variation of the SERS intensity measured as a function of the streamwise position along the microchannel, which also corresponds to nanoparticle exposure time. This allows us to monitor simultaneously the nanoparticle aggregation process and to determine the location at which the SERS signal is optimized.
View details for DOI 10.1073/pnas.0708596104
View details for Web of Science ID 000251498700007
View details for PubMedID 18025462
-
Current distribution in polymer electrolyte membrane fuel cell with active water management
JOURNAL OF POWER SOURCES
2007; 174 (1): 272-281
View details for DOI 10.1016/j.jpowsour.2007.08.059
View details for Web of Science ID 000251591000033
-
Free-solution oligonucleotide separation in nanoscale channels
ANALYTICAL CHEMISTRY
2007; 79 (21): 8316-8322
Abstract
In this paper, we report an experimental study of electrokinetic transport and separation of double-stranded deoxyribonucleic acid (dsDNA) oligonucleotides in custom-fabricated fused-silica nanochannels filled with a gel-free sodium borate aqueous buffer. Mixtures of fluorescently labeled dsDNA molecules in the range of 10-100 base pair (bp), fluorescein, and fluorescein-12-UTP (UTP) were separated in less than 120 s in channels of depth ranging from 40 to 1560 nm. We varied the channel depth and background buffer concentration to achieve a 0.006-0.2 range of Debye length-to-channel-half-depth ratio (lambdaD/h), and a 0.004-1.7 range of the ratio of length of dsDNA molecule to channel half-depth (l/h). We find observed oligonucleotide migration times depend on both l/h and lambdaD/h. Electrophoretic mobility estimates agree well with published (micrometer-scale channel) values for background electrolyte (BGE) concentrations greater than approximately 10 mM. At BGE concentrations of 1 and 5 mM, mobility estimates in our nanochannels are higher than published values. Of the cases studied, the highest separation sensitivities were achieved in 100 nm channels with 1-10 mM ion density buffers. Potential applications of this technology include rapid small-scale sequencing and other fluorescence-based oligonucleotide separation and detection assays.
View details for DOI 10.1021/ac0710580
View details for Web of Science ID 000250584800053
View details for PubMedID 17883279
-
Taylor-Aris dispersion in temperature gradient focusing
ELECTROPHORESIS
2007; 28 (14): 2333-2344
Abstract
Microfluidic temperature gradient focusing (TGF) uses an axial temperature gradient to induce a gradient in electrophoretic flux within a microchannel. When balanced with an opposing fluid flow, charged analytes simultaneously focus and separate according to their electrophoretic mobilities. We present a theoretical and experimental study of dispersion in TGF. We model the system using generalized dispersion analysis that yields a 1-D convection-diffusion equation that contains dispersion terms particular to TGF. We consider analytical solutions for the model under uniform temperature gradient conditions. Using a custom TGF experimental setup, we compare focusing measurements with the theoretical predictions. We find that the theory well represents the focusing behavior for flows within the Taylor-Aris dispersion regime.
View details for DOI 10.1002/elps.200600830
View details for Web of Science ID 000248390900001
View details for PubMedID 17578841
-
Comments on the conditions for similitude in electroosmotic flows
JOURNAL OF COLLOID AND INTERFACE SCIENCE
2007; 310 (2): 675-677
Abstract
This note provides a few comments on the conditions required for similitude between velocity and electric field in electroosmotic flows. The velocity fields of certain electroosmotic flows with relatively thin electric double layers (EDLs) are known to be irrotational in regions outside of the EDL. Under restricted conditions, the velocity field, V , can be expressed in terms of the electric field, E , as V =cE , where c is a scalar constant. The irrotationality solution is certainly unique and exact for Stokes flow, but may not be stable (or unique) for flows with Reynolds numbers significantly greater than unity.
View details for DOI 10.1016/j.jcis.2007.01.088
View details for Web of Science ID 000246459700040
View details for PubMedID 17350645
-
Engineering model of a passive planar air breathing fuel cell cathode
JOURNAL OF POWER SOURCES
2007; 167 (1): 118-129
View details for DOI 10.1016/j.jpowsour.2007.01.073
View details for Web of Science ID 000246256300019
-
Measurement of temperature and reaction species in the cathode diffusion layer of a free-convection fuel cell
JOURNAL OF THE ELECTROCHEMICAL SOCIETY
2007; 154 (9): B910-B918
View details for DOI 10.1149/1.2752971
View details for Web of Science ID 000248984600013
- Microfluidic Control of Nanoparticle Aggregation for Surfaced Enhanced Raman Spectroscopy 2007
- On-Chip Electrophoresis Devices: Do’s, Don’ts, and Dooms Chips & Tips, Lab on a Chip 2007
-
An electro-osmotic fuel pump for direct methanol fuel cells
ELECTROCHEMICAL AND SOLID STATE LETTERS
2007; 10 (11): B196-B200
View details for DOI 10.1149/1.2772083
View details for Web of Science ID 000249323200007
-
Active water management for PEM fuel cells
JOURNAL OF THE ELECTROCHEMICAL SOCIETY
2007; 154 (10): B1049-B1058
View details for DOI 10.1149/1.2766650
View details for Web of Science ID 000248984700021
-
Rotational electrophoresis of striped metallic microrods
PHYSICAL REVIEW E
2007; 75 (1)
Abstract
Analytical models are developed for the translation and rotation of metallic rods in a uniform electric field. The limits of thin and thick electric double layers are considered. These models include the effect of stripes of different metals along the length of the particle. Modeling results are compared to experimental measurements for metallic rods. Experiments demonstrate the increased alignment of particles with increasing field strength and the increase in degree of alignment of thin versus thick electric double layers. The metal rods polarize in the applied field and align parallel to its direction due to torques on the polarized charge. The torque due to polarization has a second-order dependence on the electric field strength. The particles are also shown to have an additional alignment torque component due to nonuniform densities along their length. The orientation distributions of dilute suspensions of particles are also shown to agree well with results predicted by a rotational convective-diffusion equation.
View details for DOI 10.1103/PhysRevE.75.011503
View details for Web of Science ID 000243893400055
View details for PubMedID 17358156
- Ballistic Dispersion in Temperature Gradient Focusing 2007
-
Detection of 100 aM fluorophores using a high-sensitivity on-chip CE system and transient isotachophoresis
ANALYTICAL CHEMISTRY
2007; 79 (1): 345-349
Abstract
We present a highly sensitive capillary electrophoresis (CE) assay that combines transient, single-interface on-chip isotachophoresis (ITP) and a laser-induced confocal fluorescence detection setup. We performed experimental parametric studies to show the effects of microscope objective specifications and intensity of excitation laser on optimization of a high-sensitivity on-chip CE detection system. Using the optimized detection system, single-molecule detection of Alexa Fluor 488 was demonstrated, and signal data were validated with autocorrelation analysis. We also demonstrated a separation and detection of 100 aM fluorophores (Alexa Fluor 488 and bodipy) in a fast assay using a high-sensitivity on-chip CE detection system and an ITP/CE protocol with no manual buffer exchange steps. This is, to the knowledge of the authors, the highest electrophoretic separation sensitivity ever reported.
View details for DOI 10.1021/ac060949p
View details for Web of Science ID 000243143300050
View details for PubMedID 17194159
-
The role of ambient conditions on the performance of a planar, air-breathing hydrogen PEM fuel cell
JOURNAL OF POWER SOURCES
2006; 161 (1): 168-182
View details for DOI 10.1016/j.jpowsour.2006.03.054
View details for Web of Science ID 000241412000024
-
Water management in proton exchange membrane fuel cells using integrated electroosmotic pumping
JOURNAL OF POWER SOURCES
2006; 161 (1): 191-202
View details for DOI 10.1016/j.jpowsour.2006.03.021
View details for Web of Science ID 000241412000026
-
Optimization of a microfluidic mixer for studying protein folding kinetics
ANALYTICAL CHEMISTRY
2006; 78 (13): 4299-4306
Abstract
We have applied an optimization method in conjunction with numerical simulations to minimize the mixing time of a microfluidic mixer developed for protein folding studies. The optimization method uses a semideterministic algorithm to find the global minimum of the mixing time by varying the mixer geometry and flow conditions. We describe the minimization problem and constraints and give a brief overview of the optimization algorithm. We present results of the optimization, including the optimized geometry and parameter sensitivities, and we demonstrate the improvement in mixing performance with experiments using microfabricated mixers. The dye-quenching experiments of the original and optimized mixer designs show respective mixing times of 7 and 4 mus, a 40% reduction. The new design also provides more uniform mixing across streamlines that enter the mixer. The optimized mixer is the fastest reported continuous flow mixer for protein folding.
View details for DOI 10.1021/ac051903j
View details for Web of Science ID 000238665200014
View details for PubMedID 16808436
-
Electroosmotic pumps fabricated from porous silicon membranes
JOURNAL OF MICROELECTROMECHANICAL SYSTEMS
2006; 15 (3): 717-728
View details for DOI 10.1109/JMEMS.2006.876796
View details for Web of Science ID 000238311000030
-
A hybrid method for bubble geometry reconstruction in two-phase microchannels
EXPERIMENTS IN FLUIDS
2006; 40 (6): 847-858
View details for DOI 10.1007/s00348-006-0123-z
View details for Web of Science ID 000239549100003
-
Convective instability of electrokinetic flows in a cross-shaped microchannel
JOURNAL OF FLUID MECHANICS
2006; 555: 1-42
View details for DOI 10.1017/S0022112005008542
View details for Web of Science ID 000238236200001
-
Semi-deterministic and genetic algorithms for global optimization of microfluidic protein-folding devices
INTERNATIONAL JOURNAL FOR NUMERICAL METHODS IN ENGINEERING
2006; 66 (2): 319-333
View details for DOI 10.1002/nme.1562
View details for Web of Science ID 000236623800006
-
On-chip millionfold sample stacking using transient isotachophoresis
ANALYTICAL CHEMISTRY
2006; 78 (7): 2319-2327
Abstract
We present a simple and robust isotachophoresis (ITP) method that can be integrated with microchip-based capillary electrophoresis (CE) devices to achieve millionfold sample stacking. We performed an experimental parametric study to show the effects of initial sample ion concentration, leading ion concentration, and trailing ion concentration on ITP stacking. We also discuss the usefulness and limitations of a simple one-dimensional nondispersive model and a scaling analysis for dispersion rate. We found that a single-column ITP configuration together with electroosmotic flow suppression and high leading ion concentration provide high-performance ITP and can be integrated readily with CE separation. We demonstrated detection of trace of 100 fM Alexa Fluor 488 (signal-to-noise ratio of 11) with a concentration increase of a factor of 2 x 10(6). Application of our ITP/CE protocol to the stacking and separation of negatively charged fluorescent tracers (Alexa Fluor 488 and bodipy) resulted in a concentration increase of 6.4 x 10(4) and a signal increase of 4.5 x 10(5). The ITP/CE protocol can be performed with a standard microchannel cross design or simple flow control. The method can be implemented with available off-the-shelf chip systems using off-the-shelf voltage control systems and buffer chemistries.
View details for DOI 10.1021/ac051659w
View details for Web of Science ID 000236686600037
View details for PubMedID 16579615
-
ELECTROPHORESIS IN NANOCHANNELS
PROCEEDINGS OF THE ASME FLUIDS ENGINEERING DIVISON SUMMER CONFERENCE, VOL 2
2006: 589-593
View details for Web of Science ID 000272191800082
-
Direct water removal in gas diffusion layer of porton exchnage membrane fuel cells by a flexible electroosmotic pump
PROCEEDINGS OF THE 4TH INTERNATIONAL CONFERENCE ON FUEL CELL SCIENCE, ENGINEERING, AND TECHNOLOGY, PTS A AND B
2006: 1169-1171
View details for Web of Science ID 000249884000138
-
Electrophoresis in nanochannels: brief review and speculation.
Journal of nanobiotechnology
2006; 4: 12-?
Abstract
The relevant physical phenomena that dominate electrophoretic transport of ions and macromolecules within long, thin nanochannels are reviewed, and a few papers relevant to the discussion are cited. Sample ion transport through nanochannels is largely a function of their interaction with electric double layer. For small ions, this coupling includes the net effect of the external applied field, the internal field of the double layer, and the non-uniform velocity of the liquid. Adsorption/desorption kinetics and the effects of surface roughness may also be important in nanochannel electrophoresis. For macromolecules, the resulting motion is more complex as there is further coupling via steric interactions and perhaps polarization effects. These complex interactions and coupled physics represent a valuable opportunity for novel electrophoretic and chromatographic separations.
View details for PubMedID 17116262
-
Advanced cooling technologies for microprocessors
WORLD SCIENTIFIC PUBL CO PTE LTD. 2006: 301-313
View details for Web of Science ID 000241022300016
-
A microfabricated direct methanol fuel cell with integrated electroosmotic pump
MEMS 2006: 19TH IEEE INTERNATIONAL CONFERENCE ON MICRO ELECTRO MECHANICAL SYSTEMS, TECHNICAL DIGEST
2006: 938-941
View details for Web of Science ID 000236994500235
-
Dynamics of field-amplified sample stacking
JOURNAL OF FLUID MECHANICS
2005; 543: 57-92
View details for DOI 10.1017/S0022112005005975
View details for Web of Science ID 000233542200004
-
Electrokinetic transport in nanochannels. 1. Theory
ANALYTICAL CHEMISTRY
2005; 77 (21): 6772-6781
Abstract
Electrokinetic transport in fluidic channels facilitates control and separation of ionic species. In nanometer-scale electrokinetic systems, the electric double layer thickness is comparable to characteristic channel dimensions, and this results in nonuniform velocity profiles and strong electric fields transverse to the flow. In such channels, streamwise and transverse electromigration fluxes contribute to the separation and dispersion of analyte ions. In this paper, we report on analytical and numerical models for nanochannel electrophoretic transport and separation of neutral and charged analytes. We present continuum-based theoretical studies in nanoscale channels with characteristic depths on the order of the Debye length. Our model yields analytical expressions for electroosmotic flow, species transport velocity, streamwise-transverse concentration field distribution, and ratio of apparent electrophoretic mobility for a nanochannel to (standard) ion mobility. The model demonstrates that the effective mobility governing electrophoretic transport of charged species in nanochannels depends not only on electrolyte mobility values but also on zeta potential, ion valence, and background electrolyte concentration. We also present a method we term electrokinetic separation by ion valence (EKSIV) whereby both ion valence and ion mobility may be determined independently from a comparison of micro- and nanoscale transport measurements. In the second of this two-paper series, we present experimental validation of our models.
View details for Web of Science ID 000233125400014
View details for PubMedID 16255573
-
Electrokinetic transport in nanochannels. 2. Experiments
ANALYTICAL CHEMISTRY
2005; 77 (21): 6782-6789
Abstract
We present an experimental study of nanoscale electrokinetic transport in custom-fabricated quartz nanochannels using quantitative epifluorescence imaging and current monitoring techniques. One aim is to yield insight into electrical double layer physics and study the applicability of continuum theory to nanoscale electrokinetic systems. A second aim is to explore a new separation modality offered by nanoscale electrophoretic separations. We perform parametric variations of applied electric field, channel depth, background buffer concentration, and species valence to impose variations on zeta potential, effective mobility, and Debye length among other parameters. These measurements were used to validate a continuum theory-based analytical model presented in the first of this two-paper series. Our results confirm the usefulness of continuum theory in predicting electrokinetic transport and electrophoretic separations in nanochannels. Our model leverages independent measurements of zeta potential performed in a microchannel system at electrolyte concentrations of interest. These data yield a zeta potential versus concentration relation that is used as a boundary condition for the nanochannel electrokinetic transport model. The data and model comparisons together show that the effective mobility governing electrophoretic transport of charged species in nanochannels depends not only on ion mobility values but also on the shape of the electric double layer and analyte ion valence. We demonstrate a method we term electrokinetic separation by ion valence, whereby both ion valence and mobility may be determined independently from a comparison of micro- and nanoscale transport measurements.
View details for DOI 10.1021/ac0508346
View details for Web of Science ID 000233125400015
View details for PubMedID 16255574
-
Temperature gradient focusing in a microfluidic device
ASME-AMER SOC MECHANICAL ENG. 2005: 806-806
View details for Web of Science ID 000231839600010
-
Multiple-species model for electrokinetic instability
PHYSICS OF FLUIDS
2005; 17 (6)
View details for DOI 10.1063/1.1931727
View details for Web of Science ID 000229749500026
-
Convective and absolute electrokinetic instability with conductivity gradients
JOURNAL OF FLUID MECHANICS
2005; 524: 263-303
View details for DOI 10.1017/S0022112004002381
View details for Web of Science ID 000227786800013
-
Electrokinetic instabilities in thin microchannels
PHYSICS OF FLUIDS
2005; 17 (1)
View details for DOI 10.1063/1.1823911
View details for Web of Science ID 000226358000033
- A Multiple-Species Model for Electrokinetic Instability Physics of Fluids 2005; 6 (17): 064108(1)- 064108(17)
-
A high fidelity electrokinetic flow model for the prediction of electrophoregrams in on-chip electrophoresis applications
PROCEEDINGS OF THE ASME FLUIDS ENGINEERING DIVISION
2005; 261: 197-199
View details for Web of Science ID 000243038600025
-
Nonlinear dynamics of electrokinetic instabilities
PROCEEDINGS OF THE ASME FLUIDS ENGINEERING DIVISION
2005; 261: 209-212
View details for Web of Science ID 000243038600027
-
Convective electrokinetic flow instabilities in a cross-shaped microchannel
MICRO TOTAL ANALYSIS SYSTEMS 2004, VOL 1
2005: 623-625
View details for Web of Science ID 000228997000209
-
Non-linear stacking effects in microfluidic temperature gradient focusing
PROCEEDINGS OF THE ASME FLUIDS ENGINEERING DIVISION
2005; 261: 341-344
View details for Web of Science ID 000243038600046
-
High flow rate per power pumping of aqueous solutions and organic solvents with electroosmotic pumps
PROCEEDINGS OF THE ASME FLUIDS ENGINEERING DIVISION
2005; 261: 311-314
View details for Web of Science ID 000243038600041
-
Electrokinetic flow instabilities in microfluidic systems
MECHANICS OF THE 21ST CENTURY
2005: 343-354
View details for Web of Science ID 000231853400023
-
Microfluidic mixers for UV studies of unlabeled proteins
MICRO TOTAL ANALYSIS SYSTEMS 2004, VOL 1
2005: 539-541
View details for Web of Science ID 000228997000181
-
Microsecond mixer for kinetic studies of protein folding
CELL PRESS. 2005: 376A-376A
View details for Web of Science ID 000226378501830
-
Active water management for proton exchange membrane fuel cells using an integrated electroosmotic pump
PROCEEDINGS OF THE ASME ADVANCED ENERGY SYSTEMS DIVISION
2005; 45: 243-247
View details for Web of Science ID 000243098600027
-
Electrokinetic transport and dispersion in nanoscale channels
MICRO TOTAL ANALYSIS SYSTEMS 2004, VOL 1
2005: 402-404
View details for Web of Science ID 000228997000134
-
Femtomole mixer for microsecond kinetic studies of protein folding
ANALYTICAL CHEMISTRY
2004; 76 (24): 7169-7178
Abstract
We have developed a microfluidic mixer for studying protein folding and other reactions with a mixing time of 8 mus and sample consumption of femtomoles. This device enables us to access conformational changes under conditions far from equilibrium and at previously inaccessible time scales. In this paper, we discuss the design and optimization of the mixer using modeling of convective diffusion phenomena and a characterization of the mixer performance using microparticle image velocimetry, dye quenching, and Forster resonance energy-transfer (FRET) measurements of single-stranded DNA. We also demonstrate the feasibility of measuring fast protein folding kinetics using FRET with acyl-CoA binding protein.
View details for DOI 10.1021/ac048661s
View details for Web of Science ID 000225781700003
View details for PubMedID 15595857
-
Nucleation and growth of vapor bubbles in a heated silicon microchannel
JOURNAL OF HEAT TRANSFER-TRANSACTIONS OF THE ASME
2004; 126 (4): 497-497
View details for Web of Science ID 000223989100004
-
A laser induced cavitation pump
JOURNAL OF MICROMECHANICS AND MICROENGINEERING
2004; 14 (7): 1037-1046
View details for DOI 10.1088/0960-1317/14/7/026
View details for Web of Science ID 000223090000026
-
A review of micropumps
JOURNAL OF MICROMECHANICS AND MICROENGINEERING
2004; 14 (6): R35-R64
View details for Web of Science ID 000222318500001
-
Instability of electrokinetic microchannel flows with conductivity gradients
PHYSICS OF FLUIDS
2004; 16 (6): 1922-1935
View details for DOI 10.1063/1.1710898
View details for Web of Science ID 000221345600007
-
High-pressure electroosmotic pumps based on porous polymer monoliths
SENSORS AND ACTUATORS B-CHEMICAL
2004; 99 (1): 66-73
View details for DOI 10.1016/j.snb.2003.10.031
View details for Web of Science ID 000221398700011
-
Computational study of band-crossing reactions
JOURNAL OF MICROELECTROMECHANICAL SYSTEMS
2004; 13 (2): 310-322
View details for DOI 10.1109/JMEMS.2004.825315
View details for Web of Science ID 000220759300018
-
Optimized field amplified sample stacking for on-chip capillary electrophoresis.
AMER CHEMICAL SOC. 2004: U116-U116
View details for Web of Science ID 000223655600535
-
A method for determining electrophoretic and electroosmotic mobilities using AC and DC electric field particle displacements
JOURNAL OF COLLOID AND INTERFACE SCIENCE
2004; 269 (1): 192-204
Abstract
We have developed a method for measuring the electrophoretic mobility of submicrometer, fluorescently labeled particles and the electroosmotic mobility of a microchannel. We derive explicit expressions for the unknown electrophoretic and the electroosmotic mobilities as a function of particle displacements resulting from alternating current (AC) and direct current (DC) applied electric fields. Images of particle displacements are captured using an epifluorescent microscope and a CCD camera. A custom image-processing code was developed to determine image streak lengths associated with AC measurements, and a custom particle tracking velocimetry (PTV) code was devised to determine DC particle displacements. Statistical analysis was applied to relate mobility estimates to measured particle displacement distributions.
View details for DOI 10.1016/S0021-9797(03)00601-5
View details for Web of Science ID 000187574400026
View details for PubMedID 14651913
- Electrokinetic Flow Diagnostics Micro- and Nano-Scale Diagnostic Techniques edited by Breuer, K. New York, Springer Verlag. 2004: 1
-
Porous glass electroosmotic pumps: design and experiments
JOURNAL OF COLLOID AND INTERFACE SCIENCE
2003; 268 (1): 143-153
Abstract
An analytical model for electroosmotic flow rate, total pump current, and thermodynamic efficiency reported in a previous paper has been applied as a design guideline to fabricate porous-structure EO pumps. We have fabricated sintered-glass EO pumps that provide maximum flow rates and pressure capacities of 33 ml/min and 1.3 atm, respectively, at applied potential 100 V. These pumps are designed to be integrated with two-phase microchannel heat exchangers with load capacities of order 100 W and greater. Experiments were conducted with pumps of various geometries and using a relevant, practical range of working electrolyte ionic concentration. Characterization of the pumping performance are discussed in the terms of porosity, tortuosity, pore size, and the dependence of zeta potential on bulk ion density of the working solution. The effects of pressure and flow rate on pump current and thermodynamic efficiency are analyzed and compared to the model prediction. In particular, we explore the important tradeoff between increasing flow rate capacity and obtaining adequate thermodynamic efficiency. This research aims to demonstrate the performance of EOF pump systems and to investigate optimal and practical pump designs. We also present a gas recombination device that makes possible the implementation of this pumping technology into a closed-flow loop where electrolytic gases are converted into water and reclaimed by the system.
View details for DOI 10.1016/S0021-9797(03)00730-6
View details for Web of Science ID 000186639800019
View details for PubMedID 14611783
-
Porous glass electroosmotic pumps: theory
JOURNAL OF COLLOID AND INTERFACE SCIENCE
2003; 268 (1): 133-142
Abstract
This paper presents an analytical study of electroosmotic (EO) pumps with porous pumping structures. We have developed an analytical model to solve for electroosmotic flow rate, pump current, and thermodynamic efficiency as a function of pump pressure load for porous-structure EO pumps. The model uses a symmetric electrolyte approximation valid for the high-zeta-potential regime and numerically solves the Poisson-Boltzmann equation for charge distribution in the idealized pore geometry. Generalized scaling of pumping performance is discussed in the context of a parameterization that includes porosity, tortuosity, pore size, bulk ionic density, and the nonuniform conductivity distribution over charge layers. The model also incorporates an approximate ionic-strength-dependent zeta potential formulation.
View details for DOI 10.1016/S0021-9797(03)00731-8
View details for Web of Science ID 000186639800018
View details for PubMedID 14611782
-
Thousandfold signal increase using field-amplified sample stacking for on-chip electrophoresis
ELECTROPHORESIS
2003; 24 (19-20): 3476-3483
Abstract
Field-amplified sample stacking (FASS) leverages conductivity gradients between a volume of injected sample and the background buffer to increase sample concentration. A major challenge in applying FASS to on-chip assays is the initial setup of high-conductivity gradient boundaries in the region of the injected sample volume. We have designed, fabricated, and characterized a novel FASS-capillary electrophoresis (CE) chip design that uses a photoinitiated porous polymer structure to facilitate sample injection and flow control for high-gradient FASS. This polymer structure provides a region of high flow resistance that allows the electromigration of sample ions. We have demonstrated an electropherogram signal increase by a factor of 1100 in electrophoretic separations of fluorescein and Bodipy with, respectively, 2 microM and 1 microM initial concentrations.
View details for DOI 10.1002/elps.200305611
View details for Web of Science ID 000186457900020
View details for PubMedID 14595694
-
Particle imaging techniques for microfabricated fluidic systems
EXPERIMENTS IN FLUIDS
2003; 34 (4): 504-514
View details for DOI 10.1007/S00348-003-0588-y
View details for Web of Science ID 000183198800007
-
On-chip coupling of isoelectric focusing and free solution electrophoresis for multidimensional separations
ANALYTICAL CHEMISTRY
2003; 75 (5): 1180-1187
Abstract
We have developed an acrylic microfluidic device that sequentially couples liquid-phase isoelectric focusing (IEF) and free solution capillary electrophoresis (CE). Rapid separation (<1 min) and preconcentration (73x) of species were achieved in the initial IEF dimension. Using full-field fluorescence imaging, we observed nondispersive mobilization velocities on the order of 20 microm/s during characterization of the IEF step. This transport behavior allowed controlled electrokinetic mobilization of focused sample bands to a channel junction, where voltage switching was used to repeatedly inject effluent from the IEF dimension into an ampholyte-based CE separation. This second dimension was capable of analyzing all fluid volumes of interest from the IEF dimension, as IEF was 'parked' during each CE analysis and refocused prior to additional CE analyses. Investigation of each dimension of the integrated system showed time-dependent species displacement and band-broadening behavior consistent with IEF and CE, respectively. The peak capacity of the 2D system was approximately 1300. A comprehensive 2D analysis of a fluid volume spanning 15% of the total IEF channel length was completed in less than 5 min.
View details for DOI 10.1021/ac026239a
View details for Web of Science ID 000181259300027
View details for PubMedID 12641239
-
Silicon electroosmotic micropumps for integrated circuit thermal management
BOSTON TRANSDUCERS'03: DIGEST OF TECHNICAL PAPERS, VOLS 1 AND 2
2003: 151-154
View details for Web of Science ID 000184567300038
-
Thermodynamic efficiency of porous glass electroosmotic pumps
ADVANCES IN ELECTRONIC PACKAGING 2003, VOL 1
2003: 383-390
View details for Web of Science ID 000222624900058
- Incomplete Sensitivities in Design and Control of Fluidic Channels Computer Assisted Mechanics and Engineering Sciences 2003; 10: 201-210
-
Numerical simulation of field amplified sample stacking in microfluidic system
NANOTECH 2003, VOL 1
2003: 234-237
View details for Web of Science ID 000223045100062
-
Incomplete sensitivities for the design of minimal dispersion fluidic channels
COMPUTER METHODS IN APPLIED MECHANICS AND ENGINEERING
2003; 192 (37-38): 4131-4145
View details for DOI 10.1016/S0045-7825(03)00380-3
View details for Web of Science ID 000185304100005
-
Microfluidic flow simulation: Stacking one-dimensional study
HOUILLE BLANCHE-REVUE INTERNATIONALE DE L EAU
2003: 18-23
View details for Web of Science ID 000187073700001
- Particle Tracking Techniques for Microfabricated Fluidic Systems Experiments in Fluids 2003; 4 (34): 504-513
-
Experimental study on two-phase heat transfer in microchannel heat sinks with hotspots
NINETEENTH ANNUAL IEEE SEMICONDUCTOR THERMAL MEASUREMENT AND MANAGEMENT SYMPOSIUM
2003: 242-246
View details for Web of Science ID 000182024200038
-
A planar electroosmotic micropump
JOURNAL OF MICROELECTROMECHANICAL SYSTEMS
2002; 11 (6): 672-683
View details for DOI 10.1109/JMEMS.2002.805055
View details for Web of Science ID 000179740900007
-
Photobleached-fluorescence imaging of microflows
EXPERIMENTS IN FLUIDS
2002; 33 (4): 545-554
View details for DOI 10.1007/s00348-002-0486-8
View details for Web of Science ID 000179003400007
-
Closed-loop electroosmotic microchannel cooling system for VLSI circuits
IEEE-INST ELECTRICAL ELECTRONICS ENGINEERS INC. 2002: 347-355
View details for DOI 10.1109/TCAPT.2002.800599
View details for Web of Science ID 000180333200003
-
Design and optimization of on-chip capillary electrophoresis
ELECTROPHORESIS
2002; 23 (16): 2729-2744
Abstract
We present a systematic, experimentally validated method of designing electrokinetic injections for on-chip capillary electrophoresis applications. This method can be used to predict point-wise and charge-coupled device (CCD)-imaged electropherograms using estimates of species mobilities, diffusivities and initial sample plug parameters. A simple Taylor dispersion model is used to characterize electrophoretic separations in terms of resolution and signal-to-noise ratio (SNR). Detection convolutions using Gaussian and Boxcar detector response functions are used to relate optimal conditions for resolution and signal as a function of relevant system parameters including electroosmotic mobility, sample injection length, detector length scale, and the length-to-detector. Analytical solutions show a tradeoff between signal-to-noise ratio and resolution with respect to dimensionless injection width and length to the detector. In contrast, there is no tradeoff with respect to the Peclet number as increases in Peclet number favor both SNR and separation solution (R). We validate our model with quantitative epifluorescence visualizations of electrophoretic separation experiments in a simple cross channel microchip. For the pure advection regime of dispersion, we use numerical simulations of the transient convective diffusion processes associated with electrokinetics together with an optimization algorithm to design a voltage control scheme which produces an injection plug that has minimal advective dispersion. We also validate this optimal injection scheme using fluorescence visualizations. These validations show that optimized voltage scheme produces injections with a standard deviation less than one-fifth of the width of the microchannel.
View details for Web of Science ID 000177888500022
View details for PubMedID 12210178
-
Particle tracking techniques for electrokinetic microchannel flows
ANALYTICAL CHEMISTRY
2002; 74 (15): 3704-3713
Abstract
We have applied particle tracking techniques to obtain spatially resolved velocity measurements in electrokinetic flow devices. Both micrometer-resolution particle image velocimetry (micro-PMV) and particle tracking velocimetry (PTV) techniques have been used to quantify and study flow phenomena in electrokinetic systems applicable to microfluidic bioanalytical devices. To make the flow measurements quantitative, we performed a series of seed particle calibration experiments. First, we measure the electroosmotic wall mobility of a borosilicate rectangular capillary (40 by 400 microm) using current monitoring. In addition to this wall mobility characterization, we apply PTV to determine the electrophoretic mobilities of more than 1,000 fluorescent microsphere particles in aqueous buffer solutions. Particles from this calibrated particle/ buffer mixture are then introduced into two electrokinetic flow systems for particle tracking flow experiments. In these experiments, we use micro-PIV, together with an electric field prediction, to obtain electroosmotic flow bulk fluid velocity measurements. The first example flow system is a microchannel intersection where we demonstrate a detailed documentation of the similitude between the electrical fields and the velocity fields in an electrokinetic system with uniform zeta potential, zeta. In the second system, we apply micro-PIV to a microchannel system with nonuniform zeta. The latter experiment provides a simultaneous measurement of two distinct wall mobilities within the microchannel.
View details for DOI 10.1021/ac011243s
View details for Web of Science ID 000177239200027
View details for PubMedID 12175157
-
Electroosmotic flow pumps with polymer frits
SENSORS AND ACTUATORS B-CHEMICAL
2002; 82 (2-3): 209-212
View details for Web of Science ID 000174483000010
-
Measurements and modeling of two-phase flow in microchannels with nearly constant heat flux boundary conditions
JOURNAL OF MICROELECTROMECHANICAL SYSTEMS
2002; 11 (1): 12-19
View details for Web of Science ID 000173751000002
-
Transient and sub-atmospheric performance of a closed-loop electroosmotic microchannel cooling system
THERMAL CHALLENGES IN NEXT GENERATION ELECTRONIC SYSTEMS
2002: 133-139
View details for Web of Science ID 000181956000016
- Electroosmotic microchannel cooling system for microprocessors Electronics Cooling 2002; 8: 46-47
- Bleached-Fluorescence Imaging of Microflows Experiments in Fluids 2002; 4 (33): 545-554
-
Enhanced nucleate boiling in microchannels
FIFTEENTH IEEE INTERNATIONAL CONFERENCE ON MICRO ELECTRO MECHANICAL SYSTEMS, TECHNICAL DIGEST
2002: 89-92
View details for Web of Science ID 000174908700022
-
Electrokinetic instability micromixing
ANALYTICAL CHEMISTRY
2001; 73 (24): 5822-5832
Abstract
We have developed an electrokinetic process to rapidly stir micro- and nanoliter volume solutions for microfluidic bioanalytical applications. We rapidly stir microflow streams by initiating a flow instability, which we have observed in sinusoidally oscillating, electroosmotic channel flows. As the effect occurs within an oscillating electroosmotic flow, we refer to it here as an electrokinetic instability (EKI). The rapid stretching and folding of material lines associated with this instability can be used to stir fluid streams with Reynolds numbers of order unity, based on channel depth and rms electroosmotic velocity. This paper presents a preliminary description of the EKI and the design and fabrication of two micromixing devices capable of rapidly stirring two fluid streams using this flow phenomenon. A high-resolution CCD camera is used to record the stirring and diffusion of fluorescein from an initially unmixed configuration. Integration of fluorescence intensity over measurement volumes (voxels) provides a measure of the degree to which two streams are mixed to within the length scales of the voxels. Ensemble-averaged probability density functions and power spectra of the instantaneous spatial intensity profiles are used to quantify the mixing processes. Two-dimensional spectral bandwidths of the mixing images are initially anisotropic for the unmixed configuration, broaden as the stirring associated with the EKI rapidly stretches and folds material lines (adding high spatial frequencies to the concentration field), and then narrow to a relatively isotropic spectrum at the well-mixed conditions.
View details for DOI 10.1021/ac0155411
View details for Web of Science ID 000172884900007
View details for PubMedID 11791550
-
Fabrication and characterization of electroosmotic micropumps
SENSORS AND ACTUATORS B-CHEMICAL
2001; 79 (2-3): 107-114
View details for Web of Science ID 000171679600004
-
Electroosmotic flows in microchannels with finite inertial and pressure forces
ANALYTICAL CHEMISTRY
2001; 73 (10): 2353-2365
Abstract
Emerging microfluidic systems have spurred an interest in the study of electrokinetic flow phenomena in complex geometries and a variety of flow conditions. This paper presents an analysis of the effects of fluid inertia and pressure on the velocity and vorticity field of electroosmotic flows. In typical on-chip electrokinetics applications, the flow field can be separated into an inner flow region dominated by viscous and electrostatic forces and an outer flow region dominated by inertial and pressure forces. These two regions are separated by a slip velocity condition determined by the Helmholtz-Smoulochowski equation. The validity of this assumption is investigated by analyzing the velocity field in a pressure-driven, two-dimensional flow channel with an impulsively started electric field. The regime for which the inner/outer flow model is valid is described in terms of nondimensional parameters derived from this example problem. Next, the inertial forces, surface conditions, and pressure-gradient conditions for a full-field similarity between the electric and velocity fields in electroosmotic flows are discussed. A sufficient set of conditions for this similarity to hold in arbitrarily shaped, insulating wall microchannels is the following: uniform surface charge, low Reynolds number, low Reynolds and Strouhal number product, uniform fluid properties, and zero pressure differences between inlets and outlets. Last, simple relations describing the generation of vorticity in electroosmotic flow are derived using a wall-local, streamline coordinate system.
View details for Web of Science ID 000168708200030
View details for PubMedID 11393863
-
Simulation and design of extraction and separation fluidic devices
ESAIM-MATHEMATICAL MODELLING AND NUMERICAL ANALYSIS-MODELISATION MATHEMATIQUE ET ANALYSE NUMERIQUE
2001; 35 (3): 513-523
View details for Web of Science ID 000169197700006
-
Optimization of turn geometries for microchip electrophoresis
ANALYTICAL CHEMISTRY
2001; 73 (6): 1350-1360
View details for Web of Science ID 000167546400042
-
Two-phase microchannel heat sinks for an electrokinetic VLSI chip cooling system
SEVENTEENTH ANNUAL IEEE SEMICONDUCTOR THERMAL MEASUREMENT AND MANAGEMENT SYMPOSIUM, PROCEEDINGS 2001
2001: 153-157
View details for Web of Science ID 000168411800021
- Liquid Flows in Microchannels CRC Handbook of MEMS edited by Gad-el-Hak, M. CRC Press, New York. 2001: 6-1 to 6-38
-
Modeling of two-phase microchannel heat sinks for VLSI chips
14TH IEEE INTERNATIONAL CONFERENCE ON MICRO ELECTRO MECHANICAL SYSTEMS, TECHNICAL DIGEST
2001: 422-426
View details for Web of Science ID 000166833600102
-
A micromachined silicon low-voltage parallel-plate electrokinetic pump
TRANSDUCERS '01: EUROSENSORS XV, DIGEST OF TECHNICAL PAPERS, VOLS 1 AND 2
2001: 920-923
View details for Web of Science ID 000172547800211
-
Passive mixing in a three-dimensional serpentine microchannel
JOURNAL OF MICROELECTROMECHANICAL SYSTEMS
2000; 9 (2): 190-197
View details for Web of Science ID 000087842600004
-
A PIV algorithm for estimating time-averaged velocity fields
JOURNAL OF FLUIDS ENGINEERING-TRANSACTIONS OF THE ASME
2000; 122 (2): 285-289
View details for Web of Science ID 000167106000008
-
Particle-image velocimetry measurements in electrokinetic flow.
AMER CHEMICAL SOC. 2000: U578-U578
View details for Web of Science ID 000087246103124
-
Mixing of a sonic transverse jet injected into a supersonic flow
AIAA JOURNAL
2000; 38 (3): 470-479
View details for Web of Science ID 000085771400012
-
Electroosmotic capillary flow with nonuniform zeta potential
ANALYTICAL CHEMISTRY
2000; 72 (5): 1053-1057
View details for Web of Science ID 000085605100043
-
Electroosmotic capillary flow with nonuniform zeta potential
Analytical chemistry
2000; 72 (5): 1053-7
Abstract
The present work is an analytical and experimental study of electroosmotic flow (EOF) in cylindrical capillaries with nonuniform wall surface charge (zeta-potential) distributions. In particular, this study investigates perturbations of electroosmotic flow in open capillaries that are due to induced pressure gradients resulting from axial variations in the wall zeta-potential. The experimental inquiry focuses on electroosmotic flow under a uniform applied field in capillaries with an EOF-suppressing polymer adsorbed onto various fractions of the total capillary length. This fractional EOF suppression was achieved by coupling capillaries with substantially different zeta-potentials. The resulting flow fields were imaged with a nonintrusive, caged-fluorescence imaging technique. Simple analytical models for the velocity field and rate of sample dispersion in capillaries with axial zeta-potential variations are presented. The resulting induced pressure gradients and the associated band-broadening effects are of particular importance to the performance of chemical and biochemical analysis systems such as capillary electrokinetic chromatography and capillary zone electrophoresis.
View details for PubMedID 10739211
-
Fabrication and characterization of electrokinetic micro pumps
ITHERM 2000: SEVENTH INTERSOCIETY CONFERENCE ON THERMAL AND THERMOMECHANICAL PHENOMENA IN ELECTRONIC SYSTEMS, VOL 2, PROCEEDINGS
2000: 31-36
View details for DOI 10.1109/ITHERM.2000.866167
View details for Web of Science ID 000089141400006
-
Micron-resolution velocimetry techniques
LASER TECHNIQUES APPLIED TO FLUID MECHANICS
2000: 57-70
View details for Web of Science ID 000087171900004
-
Miniaturized capillary isoelectric focusing (cIEF): Towards a portable high-speed separation method
MICRO TOTAL ANALYSIS SYSTEMS 2000, PROCEEDINGS
2000: 367-370
View details for Web of Science ID 000167335400085
-
Experimental investigation of flow transition in microchannels using micron-resolution particle image velocimetry
ITHERM 2000: SEVENTH INTERSOCIETY CONFERENCE ON THERMAL AND THERMOMECHANICAL PHENOMENA IN ELECTRONIC SYSTEMS, VOL 2, PROCEEDINGS
2000: 148-153
View details for Web of Science ID 000089141400023
-
Designing corner compensation for electrophoresis in compact geometries
MICRO TOTAL ANALYSIS SYSTEMS 2000, PROCEEDINGS
2000: 287-290
View details for Web of Science ID 000167335400065
-
PIV measurements of a microchannel flow
EXPERIMENTS IN FLUIDS
1999; 27 (5): 414-419
View details for Web of Science ID 000083322200005
- Diagnostic Techniques for Microfluidics Research Developments in Laser Techniques and Applications to Fluid Mechanics edited by Adrian, R., J., Durao, D., F.G., Durst, F. Springer-Verlag, Berlin. 1999: 1
-
A particle image velocimetry system for microfluidics
EXPERIMENTS IN FLUIDS
1998; 25 (4): 316-319
View details for Web of Science ID 000076240500004
-
Micro-resolution particle image velocimetry
MICRO- AND NANOFABRICATED STRUCTURES AND DEVICES FOR BIOMEDICAL ENVIRONMENTAL APPLICATIONS
1998; 3258: 122-133
View details for Web of Science ID 000073452100015
-
Crossflow vortices of a jet injected into a supersonic crossflow
AIAA JOURNAL
1997; 35 (5): 915-917
View details for Web of Science ID A1997WY03000024
-
Velocity measurements of a jet injected into a supersonic crossflow
JOURNAL OF PROPULSION AND POWER
1997; 13 (2): 264-273
View details for Web of Science ID A1997WN15600015
- Velocity Measurements of a Jet Injected into a Supersonic Crossflow Journal of Propulsion and Power 1997; 2 (13): 264-273
- Crossflow Vortices of a Jet Injected into a Supersonic Crossflow AIAA Journal 1997; 5 (35): 915-917