Joint use of dual-frequency electrowetting and interferometry in a digital microsystem : application to evaporation and surface ageing at drop scale / Electromouillage bi-fréquence et interférométrie : évaporation et vieillissement biochimique à l’échelle d’une goutte

Theisen, Johannes

05 February 2013

La recherche développée durant cette thèse constitue la première étape de développement d’une nouvelle méthodologie de détection sans marquage à l’échelle d’une goutte : un nouveau mécanisme de transduction est développé, basé sur l’actuation par électromouillage bi-fréquence d’un réseau d’ondes capillaires à la surface d’une goutte. La résonance capillaire de la goutte est étudiée par détection interférométrique de son apex en mouvement.La faisabilité de cette méthodologie est prouvée en caractérisant la cinétique d’évaporation de la goutte par glissement spectral des ondes capillaires.La deuxième partie de la thèse porte sur la modélisation du transport de biomolécules tensioactives dans une goutte : le transport diffusif, les processus d’ad/désorption aux surfaces, la condition cinématique d’un rayon variable(évaporation) ainsi qu’une quantité molaire finie de biomolécules sont pris en compte. Un nouveau nombre adimensionnel est proposé pour rendre compte de la taille finie d’une goutte. Puis le transport chimique associé au courant de dérive induit par les ondes capillaires (excitées par électromouillage oscillatoire)est pris en compte à l’aide de simulations numériques. Finalement,l’électromouillage haute et basse fréquence est appliqué au cas d’une goutte enrichie par des molécules d’albumine de sérum bovin. En utilisant conjointement l’interférométrie optique et l’imagerie, et en considérant la loi de Lippmann-Young, le vieillissement biochimique de la surface solide mouillée par la goutte est détecté. / This PhD research is thought of as a first step towards label freedigital biosensing. A novel transduction mechanism is developed, based on thegeneration of capillary waves along a drop surface induced by dual-frequencyelectrowetting. Acapillary resonance is measured by interferometry at the movingdrop apex. Aproof of concept of this electro-optical methodology for furtherintegration in a digital microsystem is given with characterization of drop evaporationkinetics. A second part focuses on modeling and numerical calculationsof the transport of surface active biomolecules in the drop. The model includesdiffusion, ad-/desorption phenomena together with a kinematic condition of avariable drop radius (evaporation) as well as a finite molecular amount of surfaceactive biomolecules. A dimensionless number is suggested to take into accountfinite size effects. Drop steady streaming due to oscillating electrowetting isfinally taken into account. Low- and high-frequency electrowetting is appliedto a drop laden with bovine serum albumin. By jointly using interferometry andimaging, enhancement of surface ageing is made evident under electrowetting.

Microfluidique digitale

Gouttes

Electromouillage

Interférométrie

Diffusion

Convection

Physico-sorption

Evaporation

Biomolécules

Digital microfluidics

Drops

Electrowetting

Interferometry

Diffusion

Convection

Physico-sorption

Evaporation

Biomolecules

620

A Study of Liquid Bridge Dynamics: an Application to Micro-Assembly/Une Etude de la Dynamique du Pont Liquide: une Application au Micro-Assemblage

Valsamis, Jean-Baptiste

31 May 2010

Micro-assembly processes suffer from some breaches due to the continuing trend towards an increase in the production capabilities as well as in the size reduction of the components manipulated. Usual manipulating schemes have reached their limit and capillary forces constitute a valuable alternative strategy. The goal of this work is to describe the dynamics of liquid bridges in the application of micro-assembly processes. The description is obtained using the Kelvin-Voigt model, with a spring, a damper, and a mass connected in parallel, supported by numerical simulations, analytical approximations and experiments. The works is divided into three parts. First we present important aspects of microfluidics, as well as the constitutive equations and an overview of numerical approaches used to describe fluid flow problems with moving interfaces. The second part is devoted to the capillary rise case, intended to validate and to compare the numerical approaches to analytical laws and experimental results. The implementation of the slipping and the dynamic contact angles is discussed. The last part focuses on the dynamics of the liquid bridge. The liquid bridge is confined between two circular and parallel plates and presents an axial symmetry. The description reveals that the stiffness depends on the surface tension and on the shape of the air/liquid interface, the damping coefficient depends on the viscosity and the volume of liquid and the equivalent mass depends on the density and the volume.

Kelvin-Voigt model

weak formulation

Navier-Stokes

moving mesh

level set

finite element method

capillary forces

free surface

microfluidics

surface tension

Developing New Strategies for the Preparation of Micro- and Nano-structured Polymer Materials

Nie, Zhihong

19 January 2009

This thesis described the development of new strategies for the preparation of micro- and nano-structured polymer materials. In particular, this thesis focused on: i) the synthesis of polymer particles in microreactors, and ii) the self-assembly of inorganic nanorods. First, this thesis presented the synthesis of polymer particles and capsules with pre-determined sizes and narrow size distributions (CV<2%) in continuous microfluidic reactors. The method includes (i) the emulsification of monomers in a microfluidic flow-focusing device and (ii) in-situ solidification of droplets via photopolymerization. This microfluidic synthesis provides a novel strategy for the control over the shapes, compositions, and morphologies of polymer particles. In particular, we demonstrated the control over particle shapes by producing polymer ellipsoids, disks, rods, hemispheres, plates, and bowls. We produced polymer particles loaded with dyes, liquid crystals, quantum dots, and magnetic nanoparticles. We generated core-shell particles, microcapsules, Janus and three-phasic polymer particles. Control over the number of cores per droplet was achieved by manipulating the flow rates of liquids in the microchannels. We further investigated the hydrodynamic mechanism underlying the emulsification of droplets, which helps in guiding scientists and engineers to utilize this technique. Second, we described the self-assembly of inorganic nanorods by using a striking analogy between amphiphilic ABA triblock copolymers and the hydrophilic nanorods tethered with hydrophobic polystyrene chains at both ends. We organized metal nanorods in structures with various geometries such as nanorings, nanochains, bundles, bundled nanochains, and nanospheres by tuning solely the quality of solvents. The self-assembly was tunable and reversible. This approach paved the way for the organization of anisotropic nanoparticles by using the strategies that are well-established for the self-assembly of block copolymers. We further described a systematic study of the self-assembly of polymer-tethered gold nanorods as a function of solvent composition in the system and the molecular weight of the polystyrene blocks. We found that the structure of the polymer pom-poms played an important role on the organization of polymer-tethered gold NRs. The 'supramolecular' assembly was governed by the competition between the end-to-end and side-by-side association of NRs and resulted in the controlled variation of the plasmonic properties of NRs, reflected in a 3-D plasmonic graph.

0495

Developing New Strategies for the Preparation of Micro- and Nano-structured Polymer Materials

Nie, Zhihong

19 January 2009

This thesis described the development of new strategies for the preparation of micro- and nano-structured polymer materials. In particular, this thesis focused on: i) the synthesis of polymer particles in microreactors, and ii) the self-assembly of inorganic nanorods. First, this thesis presented the synthesis of polymer particles and capsules with pre-determined sizes and narrow size distributions (CV<2%) in continuous microfluidic reactors. The method includes (i) the emulsification of monomers in a microfluidic flow-focusing device and (ii) in-situ solidification of droplets via photopolymerization. This microfluidic synthesis provides a novel strategy for the control over the shapes, compositions, and morphologies of polymer particles. In particular, we demonstrated the control over particle shapes by producing polymer ellipsoids, disks, rods, hemispheres, plates, and bowls. We produced polymer particles loaded with dyes, liquid crystals, quantum dots, and magnetic nanoparticles. We generated core-shell particles, microcapsules, Janus and three-phasic polymer particles. Control over the number of cores per droplet was achieved by manipulating the flow rates of liquids in the microchannels. We further investigated the hydrodynamic mechanism underlying the emulsification of droplets, which helps in guiding scientists and engineers to utilize this technique. Second, we described the self-assembly of inorganic nanorods by using a striking analogy between amphiphilic ABA triblock copolymers and the hydrophilic nanorods tethered with hydrophobic polystyrene chains at both ends. We organized metal nanorods in structures with various geometries such as nanorings, nanochains, bundles, bundled nanochains, and nanospheres by tuning solely the quality of solvents. The self-assembly was tunable and reversible. This approach paved the way for the organization of anisotropic nanoparticles by using the strategies that are well-established for the self-assembly of block copolymers. We further described a systematic study of the self-assembly of polymer-tethered gold nanorods as a function of solvent composition in the system and the molecular weight of the polystyrene blocks. We found that the structure of the polymer pom-poms played an important role on the organization of polymer-tethered gold NRs. The 'supramolecular' assembly was governed by the competition between the end-to-end and side-by-side association of NRs and resulted in the controlled variation of the plasmonic properties of NRs, reflected in a 3-D plasmonic graph.

0495

Microfluidic-Based In-Situ Functionalization for Detection of Proteins in Heterogeneous Immunoassays

Asiaei, Sasan

January 2013

One the most daunting technical challenges in the realization of biosensors is functionalizing transducing surfaces for the detection of biomolecules. Functionalization is defined as the formation of a bio-compatible interface on the transducing surfaces of bio-chemical sensors for immobilizing and subsequent sensing of biomolecules. The kinetics of functionalization reactions is a particularly important issue, since conventional functionalization protocols are associated with lengthy process times, from hours to days. The objective of this thesis is the improvement of the functionalization protocols and their kinetics for biosensing applications. This objective is realized via modeling and experimental verification of novel functionalization techniques in microfluidic environments. The improved functionalization protocols using microfluidic environments enable in-situ functionalization, which reduces the processing times and the amount of reagents consumed, compared to conventional methods. The functionalization is performed using self-assembled monolayers (SAMs) of thiols. The thiols are organic compounds with a sulphur group that assists in the chemisorption of the thiol to the surface of metals like gold. The two reactions in the functionalization process examined in this thesis are the SAM formation and the SAM/probe molecule conjugation. SAM/probe molecule conjugation is the chemical treatment of the SAM followed by the binding of the probe molecule to the SAM. In general, the probe molecule is selective in binding with a given biomolecule, called the target molecule. Within this thesis, the probe molecule is an antibody and the target molecule is an antigen. The kinetics of the reaction between the probe (antibody) and the target biomolecule (antigen) is also studied. The reaction between an antigen and its antibody is called the immunoreaction. The biosensing technique that utilizes the immunoreaction is immunoassay. A numerical model is constructed using the finite element method (FEM), and is used to study the kinetics of the functionalization reactions. The aim of the kinetic studies is to achieve both minimal process times and reagents consumption. The impact of several important parameters on the kinetics of the reactions is investigated, and the trends observed are explained using kinetic descriptive dimensionless numbers, such as the Damköhler number and the Peclet number. Careful numerical modeling of the reactions contributes to a number of findings. A considerably faster than conventional SAM formation protocol is predicted. This fast-SAM protocol is capable of reducing the process times from the conventional 24-hours to 15 minutes. The numerical simulations also predict that conventional conjugation protocols result in the overexposure of the SAM and the probe molecule to the conjugation reagents. This overexposure consequently lowers conjugation efficiencies. The immunoreaction kinetics of a 70 kilo-Dalton heat shock protein (HSP70) with its antibody in a hypothetical microchannel is also investigated through the FEM simulations. Optimal reaction conditions are determined, including the flow velocity and the surface concentration of the immobilized probes (antibodies). Based on the numerical results and a series of experimental studies, the fast-SAM protocol application is successfully confirmed. Moreover, the optimum reagent concentration for a given one- hour conjugation process time is determined. This functionalization protocol is successfully applied to immobilize the HSP70 antibody on gold surfaces. The use of the fast-SAM protocol and the predicted optimum conjugation conditions result in binding of the HSP70 antibody on gold, with the same or superior immobilization quality, compared to the conventional protocols. Upon implementation of a 70 μm.s^(-1) flow velocity, the reaction is observed to complete in around 30-35 minutes, which is close to the numerically predicted 30 minutes and 16 seconds. This immunoreaction time is considerably less than conventional 4-12 hour processes. The modified in-situ functionalization techniques achieved here are promising for substantially reducing the preparation times and improving the performance of biosensors, in general, and immunoassays, in particular.

Microfluidics

Functionalization

Self-assembled monolayers

Immunoreaction

Antibody conjugation

Reaction kinetics

Dimensional analysis

Finite element modeling

Atomic force microscopy

Quartz crystal microbalance

Fluorescent microscopy

Mechanical Engineering

Microscale measurement of kinetic binding properties of monoclonal antibodies in solution using Gyrolab

Johansson, Fredrik

January 2011

The number of monoclonal antibodies approved for therapeutic use has increased rapidlyover the last decade. As a consequence, precise and robust kinetic characterization techniquesare crucial in order to select the best suitable candidates. A kinetic characterization methodwas developed in Gyrolab with automated sample transfers. The characterization wasperformed in solution in a mixing CD, containing an integrated nanoliter mixing chamberwith affinity binding columns. Association rate constants were determined for four anti-TSHantibodies with values ranging from 3x105 M-1s-1 to 10x105 M-1s-1. The antibodies wereranked according to kass. Reproducibility

Affinity

association rate constant

Bioaffy

characterization

Gyrolab

immunoassay

kinetics

microfluidics

monoclonal antibody

screening

Bioengineering

Bioteknik

Medical engineering

Medicinsk teknik

Enzyme engineering

Enzymteknik

Immunology

Immunologi

Microfluidics for bioanalytical research : transitioning into point-of-care diagnostics

Scida, Karen

09 February 2015

In this dissertation, three different microfluidic devices with bioanalytical applications are presented. From chapter to chapter, the bioanalytical focus will gradually become the development of a point-of-care sensor platform able to yield a reliable and quantitative response in the presence of the desired target. The first device consists of photolithographically-patterned gold on glass bipolar electrodes and PDMS Y-shaped microchannels for the controlled enrichment, separation from a mixture, and delivery of two charged dyes into separate receiving microchannels. The principle for the permanent separation of these dyes is based on the concept of bipolar electrochemistry and depended on the balancing/unbalancing of convective and electromigrating forces caused by the application of a potential bias, as well as the activation/deactivation of the bipolar electrodes. Two different bipolar electrode configurations are described and fluorescence is used to optimize their efficiency, speed, and cleanliness of delivery. The second device is a DNA sensor fabricated on paper by wax printing and folding to form 3D channels. DNA is detected by strand-displacement induced fluorescence of a single-stranded DNA. A multiplexed version of this sensor is also shown where the experiment results in “OR” and “AND” Boolean logic gate operations. In addition, the nonspecific adsorption of the reagents to cellulose is studied, demonstrating that significant reduction of nonspecific adsorption and increased sensitivity can be achieved by pre-treating the substrate with bovine serum albumin and by preparing all analyte solutions with spectator DNA. The third device, also made of paper, has a novel design and uses a versatile electrochemical detection method for the indirect detection of analytes via the direct detection of AgNP labels. A proof-of-concept experiment is shown where streptavidin-coated magnetic microbeads and biotin-coated AgNPs are used to form a composite model analyte. The paper device, called oSlip, and electrochemical method used are easily coupled so the resulting sensor has a simple user-device interface. LODs of 767 fM are achieved while retaining high reproducibility and efficiency. The fourth device is the updated version of the oSlip. In this case, the objective is to show the current progress and limitations in the detection of real analytes using the oSlip device. A sandwich-type immunoassay approach is used to detect human chorionic gonadotrophin (pregnancy hormone) present in human urine. Various optimization steps are performed to obtain the ideal reagent concentrations and incubation time necessary to form the immunocomposite in one step, that is, by mixing all reagents at the same time in the oSlip. Additionally, improvements to the electrochemical detection step are demonstrated. / text

Microfluidics

Point-of-care

Bioanalytical

Sensor

Paper analytical devices

Immunoassay

Electrochemistry

Fluorescence

Bipolar electrochemistry

Bipolar electrode

DNA

Boolean logic gates

Silver nanoparticle

Magnetic microbead

Biological Matter in Microfluidic Environment - from Single Molecules to Self-Assembly / Biomaterie in mikrofluidischer Umgebung - vom Einzelmolekül zur Selbstorganisation

Köster, Sarah Friederike

13 June 2006

No description available.

530 Physik

Mathematics and Computer Science

Aktin

Kollagen

Semiflexible Polymere

Mikrofluidik

Actin

Collagen

Semiflexible Polymers

Microfluidics

42.12

33.90

Manipulation of Wetting Morphologies in Topographically Structured Substrates / Flüssigkeitsmanipulation in topographisch strukturierten Substraten

Krishnacharya

16 October 2007

No description available.

530 Physik

Mathematics and Computer Science

Mikrofluidik

Benetzung

Entnetzung

Elektrobenetzung

Instabilität

Microfluidics

Wetting

Dewetting

Electrowetting

Instability

33.05

33.61

Manipulation of Monodisperse Emulsions in Microchannels / Manipulation von monodispersen Emulsionen in Mikrokanälen

Surenjav, Enkhtuul

15 December 2008

No description available.

530 Physik

Mathematics and Computer Science

Mikrofluidik

Manipulation

Emulsion

Tropfen

Mikrokanälen

microfluidics

manipulation

emulsion

droplet

microchannels

33.05

33.60

RV 000: Kondensierte Materie {Physik}