HIGH-THROUGHPUT SCREENING STRATEGIES FOR FLAT-SHEET MEMBRANE ADSORBERS VIA A MULTI-WELL DEVICE

Arežina, Ana

January 2023

Current high-throughput screening (HTS) tools (i.e., single-use 96-well filter plate) are limited to the few membrane types that are sold commercially, restricting the ability to screen membrane materials for targeted applications. In this thesis, a multi-well device capable of screening any flat-sheet membrane was designed, where multiple devices can be stacked for extensive HTS (>32 experiments). Confocal imaging of a Natrix Q cross-section – a membrane type not sold in a commercial filter plate – was carried out after 24 h in contact with green fluorescent protein to visually confirm protein-membrane interactions. The static binding capacity (SBC) of bovine serum albumin (BSA) and Herring testes DNA was found for specific parameters: membrane type (Mustang Q, Sartobind Q, Natrix Q, Durapore), salt concentration (0, 50, 100 mM NaCl), and contact time (1 min, 4 h, 8 h, 24 h). Considering solution conditions, the highest BSA SBC was observed with Natrix Q at 0 M NaCl with a contact time of 24 h. The DNA and BSA SBC values for Natrix Q were the highest among the membrane types evaluated, demonstrating consistency with literature trends. These findings suggest that SBC experiments can predict promising membrane materials for scaled-up applications. Finally, the chromatography process was replicated in this multi-well device (Natrix Q), showing 50% BSA elution from the membrane. The results of this thesis confirmed this ability to accommodate any membrane adsorber, simultaneously compare different membrane materials, and extract the membrane for post-experimental analysis. This work’s significance was emphasized in its future potential to aid with membrane material selection, particularly with exploring the properties of next-generation membrane materials (e.g., 3D-printed membranes). Three future areas for optimization with this multi-well device were highlighted: biotherapeutic purification, sequencing of membrane materials within a process, and applying it as a tool to understand ion selectivity. / Thesis / Master of Applied Science (MASc) / Membranes are used in many industries, such as water treatment, environmental remediation, and biopharmaceuticals. In the biopharmaceutical industry, high-throughput screening (HTS) tools (e.g., filter plates), which allow for miniaturized experiments, are used to perform extensive experimental analysis to determine optimal solution conditions (e.g., pH) for biomolecule binding. Unfortunately, commercial filter plates are limited in customizability for HTS of membrane materials. To address these limitations, this thesis focuses on designing and validating a multi-well device capable of incorporating any membrane adsorber. Different biomolecules (proteins, DNA), solution conditions, and membrane materials were evaluated. The results of this thesis confirmed this ability to accommodate any membrane adsorber, simultaneously compare different membrane materials, and extract the membrane for post-experimental analysis. This work also discussed using this device for future rapid membrane material selection in multiple industries (e.g., biotherapeutics, ion extraction).

3D-printed multi-well device

high-throughput screening

biomolecule binding

membrane chromatography

membrane adsorber

confocal imaging

An Assessment of Hypocenter Errors Associated with the Seismic Monitoring of Induced Hydro-fracturing in Hydrocarbon Reservoirs

Gilliland, Ellen

17 November 2009

Expanding the standard, single-well recording geometry used to monitor seismicity during hydro-fracture treatments could provide more accurate hypocenter locations and seismic velocities, improving general reservoir characterization. However, for the real, two-well data set obtained for this project, only S-wave picks were available, and testing resulted in anomalous hypocenter location behavior. This study uses a hypocenter location algorithm and both real and synthetic data sets to investigate how the accuracy of the velocity model, starting hypocenter location, recording geometry, and arrival-time picking error affect final hypocenter locations. Hypocenter locations improved using a velocity model that closely matched the observed sonic log rather than a smoothed version of this model. The starting hypocenter location did not affect the final location solution if both starting and final locations were between the wells. Two solutions were possible when the true solution was not directly between the wells. Adding realistic random picking errors to synthetic data closely modeled the dispersed hypocenter error pattern observed in the real data results. Adding data from a third well to synthetic tests dramatically reduced location error and removed horizontal geometric bias observed in the two-well case. Seismic event data recorded during hydro-fracture treatments could potentially be used for three-dimensional joint hypocenter-velocity tomography. This would require observation wells close enough to earthquakes to record P- and S-wave arrivals or wells at orientations sufficient to properly triangulate hypocenter locations. Simulating results with synthetic tests before drilling could optimize survey design to collect data more effectively and make analysis more useful. / Master of Science

hydro-fracture treatment

hypocenter location error

hypocenter inversion algorithm

multi-well survey

velocity structure

arrival-time picking error

geometric constraint

Semi-classical approximations of Quantum Mechanical problems

Karlsson, Ulf

January 2002

No description available.

Schrödinger equation

semiclassical analysis

multi-well potential

potential wells

scale functions

spectral interval

Agmon metric

interaction matrix

hierarchical potential

Helmholtz operator

Fourier integral operator

global phase

hyperbolic

Semi-classical approximations of Quantum Mechanical problems

Karlsson, Ulf

January 2002

No description available.

Schrödinger equation

semiclassical analysis

multi-well potential

potential wells

scale functions

spectral interval

Agmon metric

interaction matrix

hierarchical potential

Helmholtz operator

Fourier integral operator

global phase

hyperbolic

Études et applications des propriétés plasmoniques des réseaux nanostructurés

Couture, Maxime

08 1900

Cette thèse porte sur l’étude des propriétés plasmoniques de réseaux nanostructurés dans le but de développer des applications de bioanalyse. L'intérêt de travailler avec ces structures est dû à leur grande sensibilité de surface, leur facilité de fabrication et leur simplicité d'analyse par spectrophotométrie en transmission. L'objectif était de fabriquer un dispositif capable d'effectuer du criblage à haut débit pour des fins biomédicales. Le premier objectif de la thèse porte sur l’étude des propriétés plasmoniques des réseaux de nanotrous. Une compréhension approfondie de ces structures a permis d’exploiter efficacement leur performance pour des applications de bioanalyse plasmonique. Une solution analytique fut établie pour étudier les modes de diffractions des polaritons de plasmons de surface d’onde de Bloch (BW-SPP). Cette équation a permis de corroborer les observations expérimentales avec des calculs théoriques par rapport au couplage plasmonique des réseaux de nanotrous. De plus, la variation de l'angle d'incidence a permis de déplacer la fréquence à laquelle les modes plasmoniques sont excités. Il était donc possible d'ajuster la position des BWSPP de façon à maximiser un couplage à une longueur d'onde désirée. Cet effet a été exploité avec la technique d'amplification de surface de diffusion Raman exaltée (SERS). Finalement, la sensibilité en surface de réseaux de nanotrous a été amplifiée selon l’angle d’excitation en transmission. Ce gain en sensibilité permet la détection de protéines d’IgG humain pour des basses concentrations de l’ordre du nanomolaire (nM). Le second objectif de la thèse traite du développement d’un lecteur multipuits couplé avec la technologie des réseaux de nanotrous afin de créer une plateforme de détection plasmonique pour du criblage à haut débit. Cet instrument offre une analyse en transmission d’échantillons nanostructurés à l’aide d’une plaque 96-puits pour des angles d’incidence allant jusqu’à 50°. Une nouvelle méthode de microfabrication de réseaux de nanotrous par photolithographie fut établie. Cette technique a permis de fabriquer des réseaux de nanotrous sur de grandes surfaces avec uniformité. L’efficacité du système fut démontrée pour la détection de protéines d’IgG humain, du méthotrexate (MTX) et le criblage d’anticorps de l’antigène prostatique spécifique (PSA). Le dernier volet de la thèse discute de l’étude des propriétés plasmoniques de réseaux de nanodisques recouverts d’un film d’or pour amplifier plus fortement la sensibilité des capteurs plasmoniques. Cette section de la thèse a démontré la performance des réseaux de nanodisques en tant que capteur plasmonique. En effet, les réseaux de nanodisques ont l’avantage d’exciter un mode de Bragg (BM, Bragg modes) en transmission directe générant une bande plasmonique fine ayant un facteur de mérite (FOM, figure of merit) élevé (sensiblité/réponse plasmonique). L’excitation de ces structures en transmission directe a simplifié énormément l’utilisation du robot multipuits par l’excitation à incidence normale tout en offrant une FOM supérieure aux réseaux de nanotrous. Pour continuer, des simulations 3D et une image Raman du signal SERS des structures ont démontré que le champ plasmonique des BM est grandement confiné autour des nanodisques. Ce confinement du champ plasmonique des réseaux de nanodisques à générer un facteur d’amplification SERS de l’ordre de 107. En somme, cette thèse démontre une étude des propriétés plasmoniques de réseaux nanostructurés pour des applications de bioanalyse par criblage à haut débit. Les études rapportées dans cette thèse ont prouvés que le champ plasmonique des réseaux de nanotrous peut être contrôlé afin d’amplifier leur sensibilité. De plus, la thèse rapporte la première plateforme de bioanalyse plasmonique utilisant un lecteur multipuits. Finalement, la fabrication de structures plasmoniques composés de nanodisques d’or a permis de mettre en évidence des propriétés optiques qui peuvent être mises à profit pour des mesures optiques ultras sensibles. / This thesis describes the plasmonic properties of nanostructured arrays towards development of biosensing applications. These structures exhibited several advantages such as high surface sensitivity, ease of microfabrication and simple excitation setup in transmission spectroscopy. The goal was to design a plasmonic device able to achieve high throughput analysis for biomedical purposes. The first section of the thesis covers a study of the plasmonic properties of nanohole arrays. An analytical solution was derived to assess plasmonic properties of the diffraction modes of Bloch-Wave surface plasmon polaritons (BW-SPP). Tuning of the excitation angle allowed for a precise control of the plasmonic signal’s position and an optimal coupling at a specific wavelength. This feature of nanohole arrays was demonstrated for applications in surface-enhanced Raman scattering (SERS). Finally, this section described the enhancement of the surface sensitivity of nanohole arrays through variation of the excitation angle in transmission. Such enhancement of the sensitivity allowed for detection of the concentration of human IgG proteins in the low nanomolar range. The second section of the thesis discusses the development of a multi-well plate reader coupled with the nanohole arrays technology. A custom-built plasmonic reader, designed at University of Montreal, allowed analysis of plasmonic structures in transmission with a 96-well plate for excitation where the incident angle is up to 50° relative to normal. A novel microfabrication technique of nanohole arrays, based on photolithography, is described. This technique allowed fabrication of nanohole arrays on a large scale with great surface uniformity. The performance of the plasmonic reader is demonstrated for sensing of human IgG proteins, methotrexate (MTX) and screening of prostate specific antigen (PSA) antibodies. The final section of the thesis describes studies on the plasmonic properties of nanodisk arrays coated with a gold film. This section described the performance of nanodisk arrays for plasmonic sensing. This structure benefited from the excitation of Bragg modes (BM) in direct transmission, which generated a sharp plasmonic band with a high figure of merit (FOM). The excitation of nanodisk arrays in direct transmission simplified the design of the plasmonic reader while providing a greater FOM than nanohole arrays. Furthermore, 3D simulations and a Raman image of the nanodisk arrays’ SERS intensity showed the confinement of the plasmonic field of the BM at the edges of the nanodisk. Such confinement of the plasmonic field of nanodisk arrays led to high SERS enhancements to a factor of 10^7. In summary, this thesis studied the plasmonic properties of nanostructured arrays towards development of applications for high throughput biosensing. These studies proved that the plasmonic field of nanohole arrays can be tuned to enhance their surface sensitivity. Furthermore, the thesis revealed the first plasmonic sensing platform using a multiwell plate reader. Finally, the thesis describes a novel plasmonic structure with outstanding optical properties; the gold coated nanodisk arrays.

Plasmonique

Réseaux de nanotrous

Réseaux de nanodisques

Biocapteur

Lecteur multipuits

SERS

Plasmonic

Nanohole arrays

Nanodisk arrays

Biosensor

Multi-well plate reader

Ultrasonic Fluid and Cell Manipulation

Ohlin, Mathias

January 2015

During the last decade, ultrasonic manipulation has matured into an important tool with a wide range of applications, from fundamental cell biological research to clinical and industrial implementations. The contactless nature of ultrasound makes it possible to manipulate living cells in a gentle way, e.g., for positioning, sorting, and aggregation. However, when manipulating cells using ultrasound, especially using high acoustic amplitudes, a great deal of heat can be generated. This constitutes a challenge, since the viability of cells is dependent on a stable physiological temperature around 37°C.      In this Thesis we present applications of ultrasonic manipulation of fluids, particles, and cells in temperature-controlled micrometer-sized devices fabricated using well established etching techniques, directly compatible with high-resolution fluorescence microscopy. Furthermore, we present ultrasonic manipulation in larger up to centimeter-sized devices optimized for fluid mixing and cell lysis. In the present work, two new ultrasonic manipulation platforms have been developed implementing temperature control. These platforms are much improved with increased performance and usability compared to previous platforms. Also, two new ultrasonic platforms utilizing low-frequency ultrasound for solubilization and cell lysis of microliter-volumed and milliliter-volumed samples have been designed and implemented.      We have applied ultrasound to synchronize the interaction between large numbers of immune, natural killer cells, and cancer cells to study the cytotoxic response, on a single cell level. A heterogeneity was found among the natural killer cell population, i.e., some cells displayed high cytotoxic response while others were dormant. Furthermore, we have used temperature-controlled ultrasound to form up to 100, in parallel, solid cancer HepG2 tumors in a glass-silicon multi-well microplate. Next, we investigated the immune cells cytotoxic response against the solid tumors. We found a correlation between the number of immune cells compared to the size of the tumor and the cytotoxic outcome, i.e., if the tumor could be defeated.             Finally, the effect of high acoustic pressure amplitudes in the MPa-range on cell viability has been studied in a newly developed platform optimized for long-term stable temperature control, independent on the applied ultrasound power. Lastly, we present two applications of ultrasonic fluid mixing and lysis of cells. One platform is optimized for small microliter-sized volumes in plastic disposable chips and another is optimized for large milliliter-sized volumes in plastic test tubes. The latter platform has been implemented for clinical sputum sample solubilization and cell lysis for genomic DNA extraction for subsequent pathogen detection / Ultraljudsmanipulering har under de senaste tio åren mognat och utvecklats till ett verktyg med ett brett användningsområde. Idag kan man finna applikationer inom allt från cellbiologisk grundforskning till industri samt sjukvård. Ultraljudsmanipuleringens kontaktlösa natur gör det till en varsam metod för att manipulera celler, till exempel inom positionering, sortering och aggregering. När ultraljud med hög amplitud används kan värmeutvecklingen, som är oundviklig, bli ett problem. För att kunna säkerställa hög cellviabilitet krävs temperaturkontroll som kan hålla en fysiologisk, stabil temperatur på 37°C.      I denna avhandling presenterar vi tillämpningar av temperaturkontrollerad ultraljudsmanipulering i mikrometerstora anordningar fabricerade med väletablerade etsningstekniker.  Dessa anordningar är optimerade för att vara fullt kompatibla med högupplöst fluorescensmikroskopi.  Vi demonstrerar även ultraljudsmanipulering i centimeterstora anordningar optimerade för omrörning och blandning av vätskor samt lysering av celler. Två nya plattformar för ultraljudsmanipulering med inbyggd temperaturkontroll har utvecklats. Dessa två plattformar erbjuder ökad prestanda, flexibilitet samt även användarvänlighet. Utöver dessa plattformar har ytterligare två anordningar för lågfrekvent ultraljudssolubilisering och cellysering av mikroliter- och milliliterstora prover konstruerats.      I denna avhandling har vi tillämpat ultraljud för att synkronisera interaktionen mellan populationer utav immunceller (natural killer-celler) och cancerceller för att på cellnivå studera det cytotoxiska gensvaret. Vi fann en heterogenitet hos immuncellspopulationen. Det manifesterade sig i en fördelning av immuncellerna, från celler med stort cytotoxiskt gensvar till inaktiva immunceller. Vi har dessutom använt temperaturkontrollerad ultrasljudsmanipulering för att skapa solida cancertumörer utav HepG2-cancerceller, upp till 100 stycken parallellt, i en multihåls-mikrotiterplatta bestående av glas och kisel. Med hjälp av dessa tumörer har vi studerat det cytotoxiska gensvaret från immuncellerna. Vi fann att förhållandet mellan antalet immunceller och storleken på tumören bestämde utfallet, det vill säga om tumören kunde bekämpas.      Vi presenterar dessutom effekten utav högamplitudsultraljudsexponering av cancerceller i en plattform speciellt designad för höga tryckamplituder med implementerad ultraljudseffektsoberoende temperaturkontroll. Slutligen presenterar vi två tillämpningar av ultraljud för vätskeblandning och cellysering. Den första tillämpningen är anpassad för små volymer i plastchip för engångsbruk och den andra är optimerad för större volymer i plastprovrör. Den senare tillämpningen är speciellt framtagen för ultraljudssolubilisering och cellysering utav kliniska sputumprover för att möjliggöra DNA-extrahering för detektion av smittämnen. / <p>QC 20150522</p>

3D cell culture

Acoustic streaming

Acoustofluidics

Cell manipulation

High-resolution imaging

Multi-well

Microplate

Natural killer cell

Piezo

Radiation force

Solid tumor

Solubilization

Spheroid

Standing wave

Temperature control

Transducer

Trapping

Ultrasonic