Effect of Micro-Particle Addition on Frictional Energy Dissipation and Strength of Concrete : Experiments and Modelling / Effet de l'addition de micro-particules sur la dissipation d'énergie et la résistance mécanique du béton : Essais et modélisation

Scerrato, Daria

07 November 2014

Si un béton classique est constitué d'éléments de granulométrie décroissante, en commençant par les granulats, le spectre granulométrique se poursuit avec la poudre de ciment puis parfois avec un matériau de granulométrie encore plus fine comme une fumée de silice (récupérée par exemple au niveau des filtres électrostatiques dans l'industrie de l'acier). L'obtention d'un spectre granulométrique continu et étendu vers les faibles granulométries permet d'améliorer la compacité, donc les performances mécaniques. L'idée de base de cette thèse a été d'utiliser comme éléments de granulométrie fine des fillers à base de calcaire. Ces fillers ont des granulométries très fines qui leur permettent de remplir les micro-fissure généralement présentes à l'intérieur du béton. La surface rugueuse des grains de ces fillers permet de modifier le coefficient de frottement entre les lèvres de chaque fissure. Le résultat souhaité est celui de produire un béton qui dissipe par frottement plus d'énergie par rapport à un béton standard. Un béton de ce type pourrait avoir des applications importantes dans l'ingénierie civile, surtout pour ce qui concerne l'absorption des vibrations dans la ville et les constructions en régions séismiques. Les théories des milieux continus généralisés permettent de tenir compte de l’effet de la microstructure des matériaux sur leur comportement macroscopique et, en particulier, de décrire la dissipation d’énergie dans le béton sujet à des chargements cycliques. Un modèle continu généralisé avec une variable cinématique supplémentaire a été développé dans le cadre de cette thèse qui permet de décrire le glissement relatif des lèvres des fissures dans le béton à l'échelle microscopique. La relation entre ces micro-mouvements au niveau des lèvres de fissures et la dissipation d'énergie observée à l'échelle macroscopique a ensuite été étudiée. Les équations en forme forte qui dérivent de cette modélisation continue sont obtenues à l'aide d'un principe variationnel de Hamilton-Rayleigh dans lequel on a intégré la nature dynamique du problème ainsi que la possibilité de décrire des phénomènes de dissipation au niveau microscopique. Le modèle obtenu permet de décrire les cycles d'hystérésis typiques du béton sujet à des chargement cycliques et ses paramètres ont été calés sur des essais menés au LGCIE de l'INSA de Lyon. Des études paramétriques concernant les paramètres reliés à la microstructure du matériau ont permis d'identifier l'effet que l'addition des micro-fillers a sur le comportement mécanique global du béton lorsque il est sujet à des chargement dynamiques. / In this thesis, a two-degrees-of-freedom, non-linear model is introduced aiming to describe internal friction phenomena which have been observed in some modified concrete specimens undergoing slow dynamic compression loads and having various amplitudes but never inducing large strains. The motivation for the theoretical effort presented here arose because of the experimental evidence described in some papers in which dissipation loops for concrete-type materials are shown to have peculiar characteristics. Since viscoelastic models –linear or non-linear– do not seem suitable to describe either qualitatively or quantitatively the measured dissipation loops, it is proposed to introduce a micro-mechanism of Coulomb-type internal dissipation associated to the relative motion of the faces of the micro-cracks present in the material. In addition, numerical simulations, showing that the proposed model is suitable to describe some of the available experimental evidences, is presented. These numerical simulations motivate further developments of the considered model and supply a tool for the design of subsequent experimental campaigns. Furthermore, the effect of micro-particle additives such as calcium carbonate on internal dissipation of concrete was experimentally investigated. The damping performance of concrete can be improved by adding to the mixture different kinds of micro-particles with suitable size which fill the pores of the matrix and change the contact interaction between internal surfaces of voids. It was determined that the energy dissipation of the concrete increases with the increasing content of micro particles at least when the concrete matrix is “soft” enough to allow microscopic motions. On the other hand, the increasing percentage of micro-particles addition can affect the mechanical strength of the material. Thus, there is a reasonable compromise in incorporating these micro-particles to obtain higher damping with- out weakening the mechanical properties. Several concrete mixes were prepared by mixing cement powder with different percentages of micro-fillers. A concrete mix without addition of micro-particles was molded as a reference material for the sake of comparison. All these specimens were tested under cyclic loading in order to evaluate energy dissipation starting from the area of a dissipation loop detected in the diagram relative to a representative cycle. The experimental determination of the dissipated energy shows a significant increase in the damping capability of the cement-based materials with micro-filler compared to the standard concrete. The experimental results presented seem to indicate that the proposed model is suitable to describe the mechanical behavior of modified and unmodified concrete, provided that the introduced parameters are suitably tuned in order to best fit the available experimental data.

Génie civil

Structures

Béton

Microstructure

Frottement

Dissipation d'énergie

Granulométrie

Microfissure

Comportement mécanique

Modélisation

Microparticule

Ciment

Vibration

Civil engineering

Structures

Concrete

Microstructure

Friction

Energy dissipation

Particle size analysis

Microcracking

Mechanical behaviour

Modelisation

Microparticle

Cement

Vibration

624.183 407 2

Microparticules polysaccharides aux propriétés antibactériennes dirigées contre S. Aureus / Polysaccharides microparticles with antibacterial properties against S. Aureus

Dammak, Ali

19 July 2017

Staphylococcus aureus a été classé parmi les bactéries les plus pathogènes du genre Staphylococcus. Ce pathogène est responsable d'infections localisées (plaies chroniques, infections sur prothèses) voire de septicémies et d’infections nosocomiales. L’objectif principal de ce projet est d’élaborer des vecteurs colloïdaux biocompatibles à base de polysaccharides, chargés en principe actif antibactérien, et ciblant spécifiquement des biofilms de S. aureus. La méthode de complexation polyélectrolytes entre polysaccharides de charge opposée (chitosane/alginate et chitosane/dextrane sulfate) a été sélectionnée pour élaborer des particules de taille micrométrique. Ces microparticules n’étant pas stables, elles ont été stabilisées par réticulation chimique. Un antibiotique à large spectre d’activité de la famille des fluoroquinolones, la ciprofloxacine, a été séquestrée dans les microparticules. Des essais microbiologiques ont été réalisés en planctonique et sur biofilms, sur une souche de S. aureus et une souche de Pseudomonas aeruginosa. La ciprofloxacine encapsulée présente une activité antibactérienne (CMI, CMB et CMEB) plus importante que la ciprofloxacine libre. Par ailleurs, les MPs à base de chitosane/alginate sont plus actives que celles constituées de chitosane/dextrane sulfate. Enfin, un greffage d’un anticorps anti-protéine A a été réalisé sur les microparticules chitosane/alginate chargées en ciprofloxacine. Ces microparticules présentent une activité antibactérienne sur le biofilm de S. aureus légèrement améliorée par rapport aux microparticules dépourvues d’anticorps. / Staphylococcus aureus has been classified as one of the most pathogenic bacteria of the Staphylococcus genus. This bacterium is responsible for localized infections (chronic wounds, infections on artificial joints) or even septicemia and nosocomial infections. The main objective of this project is to develop biocompatible colloidal vectors based on polysaccharides, loaded with antibacterial active compound, and specifically targeting Staphylococcus aureus biofilms. The polyelectrolyte complexation between polysaccharide of opposite charge (chitosan / alginate and chitosan / dextran sulfate) has been selected to produce micrometric particles. By varying the total concentration of polysaccharide and the charge ratio between polyanion and polycation, it is possible to obtain variable sizes. As these microparticles were not stable, they were stabilized by chemical crosslinking. An antibiotic of the fluoroquinolone family, ciprofloxacin, with a large spectrum of activity, was entrapped in the micoparticles. Microbiological tests were carried out in planktonics and biofilms on different strains of Staphylococcus aureus and Pseudomonas aeruginosa. Loaded ciprofloxacin exhibits greater antibacterial activity (MIC, CMB and CMEB). Moreover, the chitosan / alginate-based MPs are more active than those consisting of chitosan / dextran sulfate. Finally, a grafting of an antiprotein A antibody was carried out on chitosan / alginate microparticles loaded with ciprofloxacin. These modified microparticles exhibit a slightly improved antibacterial activity compared to loaded ciprofloxaxin microparticles whitoutantibody.

Microparticule

Complexation polyélectrolytes

Chitosane

Alginate

Dextrane sulfate

Ciprofloxacine

Ciblage

Anticorps

Protéine A

Biofilm

Staphylococcus aureus

Pseudomonas aeruginosa

Microparticle

Polyelectrolyte complexation

Chitosan

Alginate

Dextran sulfate

Ciprofloxacin

Targeting

Antibody

Protein A

Biofilm

Staphylococcus aureus

Pseudomonas aeruginosa

572.566

Heterogeneous epoxy-amine networks from the dispersion of cross-linked polymer microparticles / Réseaux époxy-amine hétérogènes à partir de dispersions de microparticules polymères réticulées

Michon, Marie-Laure

14 February 2014

Lors de cette étude, il a été étudié l'influence de l'ajout de microparticules de polymère réticulé (CPM) dans des formulations d'époxy-amine, sur la cinétique, la morphologie et les propriétés thermo-mécaniques des réseaux finaux obtenus. Tout d'abord, un protocole simple, robuste et bien contrôlé a été développé afin d’ obtenir une large gamme de taille de CPM, de Tg et de fonctionnalité amine. Ce protocole de polymérisation par précipitation, basé sur les phénomènes de séparation de phases, a également été appliqué à différentes compositions chimiques et différents monomères époxy hydrosolubles, ceci montrant les grandes possibilités de cette méthode. Une bonne interface entre les CPMs et la matrice a été recherchée en synthétisant les CPMs en excès de groupes amines. La quantification de ces groupes amines réactifs sur les CPMS était d'un grand intérêt et a donc été étudiée en profondeur. Le titrage des amines de surface a été réalisé en mettant au point un nouveau protocole qui a permis la quantification des amines primaires et secondaires sur les CPMs. Il a ensuite été mis en évidence que, bien que ces microparticules réticulées ne soient pas poreuses, des fonctions amines sont disponibles au cœur des particules et peuvent réagir avec d'autres molécules qui sont capables de diffuser dans la CPM. Il a été montré que lorsque les CPM ont été dispersées dans des mélanges d'époxy- amine, la diffusion des monomères dans le cœur de la CPM s'est produite mais différemment selon le procédé de dispersion. En effet, en utilisant le tétrahydrofurane comme solvant pour aider à la dispersion, la diffusion de la DGEBA est amplifiée et modifie les propriétés thermo-mécaniques du réseau final en modifiant le rapport stœchiométrique de la matrice. Le même phénomène a été observé mais moins amplifié lorsque les microparticules sont uniquement dispersées mécaniquement. En dispersant les CPMs dans l'amine qui est l'agent réticulant, on observe l'absorption complète de l'amine au coeur des CPMs, conduisant ainsi à la désorption de celle-ci dans une deuxième étape, permettant de créer le réseau. Ainsi, un comportement très complexe des CPM a été mis en évidence en présence des monomères et/ou solvant : le gonflement et les phénomènes de diffusion qui dépendent d'un certain nombre de paramètres tels que la température, la densité de réticulation des CPM, les paramètres de solubilité, etc. L'intensité du phénomène de diffusion conduit à une variété de comportements lorsque les CPMs sont ajoutées dans une formulation d'époxy-amine tels que: (a) une légère diminution du temps de gélification et l'augmentation de la conversion, (b) la modification de la température de transition vitreuse de la matrice. / Throughout this work, the influence of the addition of cross-linked polymer microparticles (CPMs) in epoxy-amine formulations on the kinetics, morphology and thermo-mechanical properties of the final networks have been investigated. First, an easy, robust and well-controlled protocol was developed to obtain a large range of CPM size, Tg and amine functionality. This protocol based on reaction induced phase separation via precipitation polymerization was also applied to different chemistries and water soluble epoxy pre-polymers showing the large possibilities of this method. The capacity of obtaining a good compatibility between the CPMs and the matrix was ensure by synthesizing the CPMs in excess of amino groups. The study of the remaining reactive amino groups on the CPMS was of great interest and therefore deeply investigated. The titration of the surface amine was performed by developing a new protocol that enabled the quantification of primary and secondary amines on CPMs. It was then highlighted that even though these cross-linked microparticles were not porous, amino groups are available into the core and can react with other molecules that are able to diffuse into the CPM core. It was shown that when CPMs were dispersed into epoxy-amine blends, the diffusion of monomers into the CPM core occurred but differently depending on the dispersion process. Indeed, using tetrahydrofuran as solvent to help for the dispersion increased the diffusion of DGEBA into the CPM core and changed the thermo-mechanical properties of the final network by modifying the stoichiometric ratio of the matrix. Same phenomenon was observed but less amplified when CPMs were mechanically dispersed in DGEBA. Regarding the dispersion of CPMs in the amine cross-linker, IPD, its complete absorption could be observed into the CPMs, leading then to the desorption of IPD to create the network. Thus, a very complex behavior of CPMs was highlighted in presence of monomers or/and solvent: swelling and diffusion phenomena that are dependent on a number of parameters such as temperature, CPM cross-link density, solubility parameters, etc. The intensity of those phenomena leads to a variety of behaviors when CPMs are added into an epoxy-amine formulation: (a) slight decrease of gel times and increase of conversion, (b) modification of glass transition temperature of the matrix.

Polymère thermodurcissable

Réseau epoxy-Amine

Microparticule de polymère réticulé

Polymérisation par précipitation

Gélification

Vitrification

Séparation de phase

Amine en surface

Propriété thermomécanique

Thermosetting polymer

Amine epoxy network

Crosslinked polymer microparticle

Precipitation polymerization

Gelation

Vitrification

Phase separation

Surface amine

Characterization

Thermomechanical properties

620.192 072

Targeting the Dectin-1 Receptor via Beta-Glucan Microparticles to Modulate Alternatively Activated Macrophage Activity and Inhibit Alternative Activation / INFLUENCING PROFIBROTIC MACROPHAGE POLARIZATION AND ACTIVITY USING YEAST-DERIVED MICROPARTICLES

Imran Hayat, Aaron

January 2021

Idiopathic Pulmonary Fibrosis (IPF) is a debilitating respiratory disorder that is characterized by a progressive decline in lung function. Originating through unknown etiology, it is essentially an unchecked wound healing response that causes the build-up of excessive scar tissue in the lung interstitial tissue with a heavy toll on the patient’s respiratory capacity. Pro-fibrotic alternatively activated macrophages (M2) have been linked as an important contributor to the fibrotic remodeling of the lung. Previous Ask research indicates that targeting M2 macrophages is possible through the use of the Dectin-1 receptor, a transmembrane cell surface receptor found in high abundance on M2 macrophages. Activating the Dectin-1 receptor through the use of beta-glucan, a ligand the receptor has a high affinity for, initiates a pro-inflammatory response within the naturally immunosuppressive macrophage and can alter its activity to be less fibrogenic. Our data suggest that M2 polarization of naïve macrophages can be inhibited in vitro by beta-glucan microparticles. Additionally, we have found that polarized M2 macrophages adopt M1-like characteristics when treated with beta-glucan microparticles, in a process that is largely Dectin-1 dependent. M2 cell surface marker CD206, increased levels of which are associated with rapidly progressing IPF, shows significantly decreased frequency of expression in M2 macrophages treated with beta-glucan microparticles. Our assessment for cell-specific uptake of beta-glucan microparticles suggests an important role of the Dectin-1 receptor for significantly increased uptake in murine wild-type M2 macrophages relative to their Dectin-1 knockout counterpart. The use of beta-glucan microparticles as a potential anti-fibrotic therapeutic was assessed in the bleomycin model of fibrotic lung disease. Mice given bleomycin and treated with beta-glucan displayed decreased soluble collagen content and TGFB expression within lung homogenate relative to fibrotic bleomycin control mice. Overall, these results provide insight into the use of beta-glucan as a potential activity modulator of macrophage function in IPF and the possibility of its use as a therapeutic. / Thesis / Master of Science (MSc)

PROFIBROTIC MACROPHAGE POLARIZATION AND REPROGRAMMING IN PRECISION CUT LUNG SLICES

Kumaran, Vaishnavi

January 2024

Idiopathic pulmonary fibrosis (IPF) is a progressive lung disease with worsening respiratory symptoms and physiological impairment. Pulmonary fibrosis is a chronic lung disease characterized by forming scar tissue (fibrosis) in the lungs. Alternatively activated macrophages (M2) known as pro-fibrotic are known to contribute to the fibrotic remodeling of the lung. In addition to the polarization of slices from naïve to pro-fibrotic, the addition of anti-fibrotic therapeutics reprogram slices back to a naïve condition. To polarize the slices, naïve slices are incubated with a previously investigated method in the lab known as the polarization cocktail. The polarization cocktail can be achieved by adding of IL-4, IL-6 and IL-13 to naïve(M0) slices in the Precision Cut lung slice (PCLS) model. For the therapeutic model, slices are incubated with the polarization cocktail and subsequently with the therapeutic. Our results have shown that the precision cut lung slice model can mimic previously investigated in-vivo experiments with the polarization cocktail. Secondly, the addition of therapeutics result in the slices exhibiting lower amounts of M2 markers and arginase activity concluding the model is suitable for the polarization and reprogramming of macrophages. / Thesis / Master of Science in Medical Sciences (MSMS)

Idiopathic pulmonary fibrosis

IPF

PCLS

Alternatively activated macrophage

M2

M1

Classically activated macrophage

Interstitial lung disease

Fibrotic lung disease

IHC

TGF-B

Beta-glucan

Microparticle

Yeast-Derived Beta Glucan

Ex vivo Models

Caractérisation d'une famille de récepteurs kinases impliqués dans le développement gamétophytique chez Arabidopsis thaliana

Houde, Josée

02 1900

Au cours du développement des végétaux, de l’établissement de l’identité cellulaire des premiers organes au guidage du tube pollinique, la communication cellule à cellule est d’une importance capitale. En réponse, les voies de signalisation moléculaires sont élaborées pour la perception d’un signal extérieur et la transduction en une réponse génique via une cascade intracellulaire. Les récepteurs kinases font partie des protéines perceptrices des stimuli et constituent chez les plantes une catégorie de protéines avec une occurrence considérable, mais dont très peu d’informations détaillées sont disponibles à ce jour. Une famille de récepteurs kinases chez Arabidopsis thaliana, AtORK11 (Arabidopsis thaliana Ovule Receptor Kinase 11), a été identifiée par orthologie à un récepteur spécifique aux ovaires chez une solanacéee sauvage, Solanum chacoense. La fonction présumée de cette famille de récepteurs kinases de type leucine-rich repeat, suggérée par son patron d’expression, implique les événements relatifs au développement des gamétophytes et à la reproduction. Afin de caractériser la fonction des quatre gènes de la famille (AtORK11a, AtORK11b, AtORK11c et AtORK11d) une stratégie d’analyse de mutants d’insertion de l’ADN-T et d’évaluation du mode d’action par complémentation bimoléculaire par fluorescence (BiFC) a été entreprise. Aucune fonction précise n’a pu être attribuée aux doubles mutants d’insertion, par contre la surexpression d’une construction dominante négative indique un rôle dans le développement gamétophytique. Il a aussi été démontré que les quatre récepteurs peuvent interagir par homodimérisation aussi bien que par hétérodimérisation. Une hypothèse de redondance fonctionnelle est ainsi mise à jour parmi la famille des gènes AtORK11. / Cell to cell communication is paramount during plant developmental processes, from cellular identity in early organogenesis to pollen tube guidance. In response to this requirement, molecular cell signalling is used to perceive an external signal and transduce the response by an intracellular signalling cascade leading to specific gene activation. The sensing protein is typically a receptor kinase, which will transduce the stimulus by phosphorylation of a cytoplasmic interaction partner. Although plant receptor kinases represent the largest protein kinase family, only handfuls are well characterized. By sequence identity (orthology), a family of leucine-rich repeat receptor kinases from Arabidopsis thaliana was identified as AtORK11 (Arabidopsis thaliana Ovule Receptor Kinase 11). Based upon previous results from its ortholog in Solanum chacoense, the ovary- specific ScORK11 receptor kinase, we hypothesized that members of the AtORK11 receptors would be involved in gametophyte development and reproduction. In order to characterize the role of the four family members (AtORK11a, AtORK11b, AtORK11c and AtORK11d), a T-DNA insertional mutant strategy was undertaken, as well as bimolecular fluorescence complementation assays (BiFC). No precise function could be assigned to the double mutants although a dominant negative strategy revealed an involvement in gametophytic development. It was also shown that all of the receptors could form homodimers as well as heterodimers in a heterologous system, suggesting high functional redundancy for the AtORK11 family.

transduction de signal

mutant d'insertion ADN-T

leucine-rich repeat receptor kinase

signal transduction

T-DNA insertion mutant

bimolecular fluorescence complementation

tungsten microparticle bombardment

Caractérisation d'une famille de récepteurs kinases impliqués dans le développement gamétophytique chez Arabidopsis thaliana

Houde, Josée

02 1900

Au cours du développement des végétaux, de l’établissement de l’identité cellulaire des premiers organes au guidage du tube pollinique, la communication cellule à cellule est d’une importance capitale. En réponse, les voies de signalisation moléculaires sont élaborées pour la perception d’un signal extérieur et la transduction en une réponse génique via une cascade intracellulaire. Les récepteurs kinases font partie des protéines perceptrices des stimuli et constituent chez les plantes une catégorie de protéines avec une occurrence considérable, mais dont très peu d’informations détaillées sont disponibles à ce jour. Une famille de récepteurs kinases chez Arabidopsis thaliana, AtORK11 (Arabidopsis thaliana Ovule Receptor Kinase 11), a été identifiée par orthologie à un récepteur spécifique aux ovaires chez une solanacéee sauvage, Solanum chacoense. La fonction présumée de cette famille de récepteurs kinases de type leucine-rich repeat, suggérée par son patron d’expression, implique les événements relatifs au développement des gamétophytes et à la reproduction. Afin de caractériser la fonction des quatre gènes de la famille (AtORK11a, AtORK11b, AtORK11c et AtORK11d) une stratégie d’analyse de mutants d’insertion de l’ADN-T et d’évaluation du mode d’action par complémentation bimoléculaire par fluorescence (BiFC) a été entreprise. Aucune fonction précise n’a pu être attribuée aux doubles mutants d’insertion, par contre la surexpression d’une construction dominante négative indique un rôle dans le développement gamétophytique. Il a aussi été démontré que les quatre récepteurs peuvent interagir par homodimérisation aussi bien que par hétérodimérisation. Une hypothèse de redondance fonctionnelle est ainsi mise à jour parmi la famille des gènes AtORK11. / Cell to cell communication is paramount during plant developmental processes, from cellular identity in early organogenesis to pollen tube guidance. In response to this requirement, molecular cell signalling is used to perceive an external signal and transduce the response by an intracellular signalling cascade leading to specific gene activation. The sensing protein is typically a receptor kinase, which will transduce the stimulus by phosphorylation of a cytoplasmic interaction partner. Although plant receptor kinases represent the largest protein kinase family, only handfuls are well characterized. By sequence identity (orthology), a family of leucine-rich repeat receptor kinases from Arabidopsis thaliana was identified as AtORK11 (Arabidopsis thaliana Ovule Receptor Kinase 11). Based upon previous results from its ortholog in Solanum chacoense, the ovary- specific ScORK11 receptor kinase, we hypothesized that members of the AtORK11 receptors would be involved in gametophyte development and reproduction. In order to characterize the role of the four family members (AtORK11a, AtORK11b, AtORK11c and AtORK11d), a T-DNA insertional mutant strategy was undertaken, as well as bimolecular fluorescence complementation assays (BiFC). No precise function could be assigned to the double mutants although a dominant negative strategy revealed an involvement in gametophytic development. It was also shown that all of the receptors could form homodimers as well as heterodimers in a heterologous system, suggesting high functional redundancy for the AtORK11 family.

transduction de signal

mutant d'insertion ADN-T

leucine-rich repeat receptor kinase

signal transduction

T-DNA insertion mutant

bimolecular fluorescence complementation

tungsten microparticle bombardment

OSTE Microfluidic Technologies for Cell Encapsulation and Biomolecular Analysis

Zhou, Xiamo

January 2017

In novel drug delivery system, the encapsulation of therapeutic cells in microparticles has great promises for the treatment of a range of health con- ditions. Therefore, the encapsulation material and technology are of great importance to the validity and efficiency of the advanced medical therapy. Several unsolved challenges in regards to versatile microparticle synthesis ma- terials and methods form the main obstacle for a translation of novel cell therapy concepts from research to clinical practice. Thiol-ene based polymer systems have emerged and gained great popular- ity in material development in general and in biomedical applications specif- ically. The thiol-ene platform is broad and therefore of interest for a variety of applications. At the same time, many aspects of this material platform are largely unexplored, for example material and manufacturing technology developments for microfluidic applications . In this Ph.D. thesis, thiol-ene materials are explored for use in cell encap- sulation. The marriage of these two technology fields breeds the possibility for a novel microfluidic cell encapsulation approach using a novel encapsulation material. To this end, several new manufacturing technologies for thiol-ene and thiol-ene-epoxy droplet microfluidic devices were developed. Moreover, core-shell microparticle synthesis for cell encapsulation based on a novel co- synthesis concept using a thiol-ene based material was developed and inves- tigated. Finally, a thiol-ene-epoxy system was also used for the formation of microwells and microchannels that improve protein analysis on microarrays. The first part of the thesis presents the background and state-of-the-art technologies in regards to cell therapy, microfluidics, and thiol-ene based ma- terials. In the second part of the thesis, a novel manufacturing approach of thiol-ene-epoxy material as well as core-shell particle co-synthesis in micro- fluidics using thiol-ene based material are presented and characterized. The third part of the thesis presents the cell viability studies of encapsulated cells using the novel encapsulation material and method. In the final part of the thesis, two applications of thiol-ene-epoxy gaskets for protein detection mi- croarrays are presented. / Inkapsling av levande celler i mikrokapslar för terapeutiska ändamål är mycket lovande för frmatida behandling av många olika sjukdomar. Emeller- tid är en behandlings effektivitet i hög grad beroende av vilka material som används för inkapsling och vilken teknisk lösning som används för att ska- pa mikrokapslarna. För närvarande återstår det många utmaningar för att omvandla grundforskningresultat till klinisk verklighet, vilken kräver mer än- damålsenliga tillvägagångssätt för att tillverka mikrokapslar i material som är kompatibla med användningsområdena. De senaste åren har tiol-en baserade polymerer har blivit mycket använda för materialutveckling i stort och för biomedicinska tillämpningar i synnerhet. Med tiol-en kemi kan en mycket stor mängd helt olika syntetiska material framställas, vilket gör tiol-ener intressanta för en mängd applikationer. För närvarande är dock mycket inom denna materialklass outforskat, t.ex. inom material och tillverkningmetodik för mikrofluidiktillämpningar. I denna avhandling används tiol-ener för cellinkapsling. Sammanslagning av dessa teknologier möjliggör en ny typ av cellinkapsling med nya materi- alegenskaper. En mängd olika tillverkningssätt där tiol-en eller tiol-en-epoxi används för droplet-mikrofluidiksystem utvecklades. Core-shell mikrokapsel- syntes för cell-inkapsling baserat på en ny metod för samtidig syntes av både core och shell utvecklades och karaktäriserades. Slutligen utvecklades ett tiol- en-epoxi system för enkel integrering med proteinmikroarrayer på objektsglas. I avhandlingens första del presenteras bakgrund och dagens bästa teknolo- gier för terapeutisk cellinkapsling, mikrofluidik och tiol-en baserade material. I avhandlingens andra del presenteras en ny tillverkningsmetod för mikro- strukturerade tiol-en-epoxi artiklar och samtidig syntes av core och shell för mikrokapslar med användande av mikrofluidik. I den tredje delen presenteras cellöverlevandsstudier för de celler som inkapslats med de nya materialen och de nyutvecklade metoderna. I den avslutande delen beskrivs två specifika fall där tiol-en-epoxi komponenter används för proteindetektion och mikroarrayer. / <p>QC 20171122</p>

Microfluidics

microfabrication

cell encapsulation

core-shell particle

microparticle synthesis

off-stoichiometry-thiol-ene

OSTE

OSTE+

lab-on-a-chip

surface modification

core-shell particle co-synthesis

microar- ray

micromixer

bonding

surface modification

droplet microfluidics

protein screening.

Mikrofluidik

mikrofabrikation

cellinkapsling

cores-shell kap- sel

mikrokapselsyntes

lab-on-chip

ickestökiometrisk tiol-en

OSTE

OSTE+

ytmodifiering

samtidig syntes av core-shellkapslar

mikroarray

mikromixer

sammanfogning

dropletmikrofluidik

proteindetektion.

Engineering and Technology

Teknik och teknologier

Theoretical and experimental study of non-spherical microparticle dynamics in viscoelastic fluid flows

Cheng-Wei Tai (12198344)

06 June 2022

<p>Particle suspensions in viscoelastic fluids (e.g., polymeric fluids, liquid crystalline solutions, gels) are ubiquitous in industrial processes and in biology. In such fluids, particles often acquire lift forces that push them to preferential streamlines in the flow domain. This lift force depends greatly on the fluid’s rheology, and plays a vital role in many applications such as particle separations in microfluidic devices, particle rinsing on silicon wafers, and particle resuspension in enhanced oil recovery. Previous studies have provided understanding on how fluid rheology affects the motion of spherical particles in simple viscoelastic fluid flows such as shear flows. However, the combined effect of more complex flow profiles and particle shape is still under-explored. The main contribution of this thesis is to: (a) provide understanding on the migration and rotation dynamics of an arbitrary-shaped particle in complex flows of a viscoelastic fluid, and (b) develop guidelines for designing such suspensions for general applications.</p> <p><br></p> <p>In the first part of the thesis, we develop theories based on the second-order fluid (SOF) constitutive model to provide solutions for the polymeric force and torque on an arbitrary-shaped solid particle under a general quadratic flow field. When the first and second normal stress coefficients satisfy  <strong>Ψ</strong>₁  = −2 <strong>Ψ</strong> ₂ (corotational limit), the fluid viscoelasticity modifies only the fluid pressure and we provide exact solutions to the polymer force and torque on the particle. For a general SOF with  <strong>Ψ</strong> ₁ ≠  −2 <strong>Ψ</strong> ₂, fluid viscoelasticity modifies the shear stresses, and we provide a procedure for numerical solutions. General scaling laws are also identified to quantify the polymeric lift based on different particle shapes and orientation. We find that the particle migration speed is directly proportional to the length the particle spans in the shear gradient direction (L_sg), and that polymeric torques lead to unique orientation behavior under flow.</p> <p><br></p> <p>Secondly, we investigate the migration and rotational behavior of prolate and oblate spheroids in various viscoelastic, pressure-driven flows. In a 2-D slit flow, fluid viscoelasticity causes prolate particles to transition to a log-rolling motion where the particles orient perpendicular to the flow-flow gradient plane. This behavior leads to a slower overall migration speed (i.e., lift) of prolate particles towards the flow centerline compared to spherical particles of the same volume. In a circular tube flow, prolate particles align their long axis along the flow direction due to the extra polymer torque generated by the velocity curvature in all radial directions. Again, this effect causes prolate particles to migrate slower to the flow centerline than spheres of the same volume. For oblate particles, we quantify their long-time orientation and find that they migrate slower than spheres of the same volume, but exhibit larger migration speeds than prolate particles. Lastly, we examine the effect of normal stress ratio ? <strong>α</strong>  = <strong>Ψ</strong> ₂ /<strong>Ψ</strong>₁on the particle motion and find that this parameter only quantitatively impacts the particle migration velocity but has negligible effect on the rotational dynamics. We therefore can utilize the exact solution derived under the corotational limit (?<strong>α</strong> = −1/2) for a quick and reasonable prediction on the particle dynamics.</p> <p><br></p> <p>We next experimentally investigate the migration behavior of spheroidal particles in microfluidic systems and draw comparisons to our theoretical predictions. A dilute suspension of prolate/oblate microparticles in a density-matched 8% aqueous polyvinylpyrrolidone (PVP) solution is used as the model suspension system. Using brightfield microscopy, we qualitatively confirm our theoretical predictions for flow Deborah numbers 0 < De < 0.1 – i.e., that spherical particles show faster migration speed than prolate and oblate particles of the same volume in tube flows.</p> <p><br></p> <p>We finally design a holographic imaging method to capture the 3-D position and orientation of dynamic microparticles in microfluidic flow. We adopt in-line holography setup and propose a straightforward hologram reconstruction method to extract the 3-D position and orientation of a non-spherical particle. The method utilizes image moment to locate the particle and localize the detection region. We detect the particle position in the depth direction by quantifying the image sharpness at different depth position, and uses principal component analysis (PCA) to detect the orientation of the particle. For a semi-transparent particle that produces complex diffraction patterns, a mask based on the image moment information can be utilized during the image sharpness process to better resolve the particle position.</p> <p><br></p> <p>In the last part of this thesis, we conclude our work and discuss the future research perspectives. We also comment on the possible application of current work to various fields of research and industrial processes.</p> <p><br></p>

Separation technologies

Microfluidics and nanofluidics

Polymers and plastics

Viscoelastic fluid

Microparticle

Polymer fluid

Rheology

Microfluidics

Holography

Boundary element method

Suspension

Particle focusing

Separation

DEVELOPMENT OF CONTROLLED DRUG DELIVERY SYSTEMS OF POLYMERIC NANOMEDICINES ASSOCIATED TO SCAFFOLDS FOR TISSUE REGENERATION

Rodríguez Escalona, Gabriela de Jesús

02 May 2016

[EN] Nowadays, one of the biggest concerns that permanently keep the attention of main important sectors of human society is health. Modern medical science is compromised with not only providing good adequate treatments but also effective specific solutions for each type of disease or human pathology. In this direction, innovative approaches like tissue engineering or regenerative medicine, controlled drug delivery systems and nanomedicines emerge to bring alternatives to situations hard to solve with conventional treatment and strategies, including the replacement of damaged or diseases tissues and/or organs. Specifically, this research is mainly aimed to design a combined system for controlled, stable and localized release of therapeutic agents that are able to exert their effect selectively on the area that warrants treatment. This construct will have enough versatility to be adapted to almost any kind of treatment, from cancer to tissue regeneration, always that the key requirement of the treatment was the need to provide the treatment of localized, stable and controlled manner. With the purposes of making easier the understanding as well as the design of the system, I was decided, for the proof of concept, to use drugs and materials with known activity applied on tissue regeneration and for the treatment of chronic wounds. The system in question consists of three main elements: 1) The first element is the polymer conjugates of therapeutic agents, which contribute to increasing the selectivity of the therapeutic action of the drug, as well as improved stability, bioavailability and biocompatibility thereof. If the drug is hydrophobic, conjugation contributes to increase its solubility in water, and in the case of proteins used as therapeutic agents, the combination helps reduce the body's immune response, increasing the chance of successful of the treatment. 2) The second element are the biodegradable polymeric microparticles, which in this case act like encapsulation agents for polymeric conjugate , thus allowing to have a second control point in the release kinetics of the therapeutic agents . Simultaneously, the microparticles also play a role in modifying the texture of the final construct, ascribing mechanical and physicochemical properties that help to improve some biological properties of the final material, such as the affinity, adhesion and cell proliferation. 3) The third element consists of a nanoporous membrane made of a biodegradable polymer by electrospinning, which constitute the unifier element of the whole system. This membrane provides manageability to the construct and is itself the last point of control in the release kinetics of the therapeutic agent or agents. Besides, it must be biocompatible and stable at ambient conditions, since this probably is going to be exposed to the environment while protecting the wound, in the case of this kind of application. These three elements, which themselves are complex systems separately, are systematically combined to achieve a synergistic relationship between them so that each one power the qualities of the other two. The resulting construct was characterized and it demonstrated to have characteristic properties that can be used as a control parameter during manufacture of this new material. Also, preliminary biological studies developed "in vitro" indicated that the proposed system may be a good candidate for deeper studies as alternative treatment for chronic wounds and other pathologies that require localized administration for long periods of time. / [ES] Actualmente, una de las mayores preocupaciones que permanentemente laman la atención de los principales sectores de la sociedad humana es la salud. La ciencia médica moderna está comprometida no solo con suministrar tratamientos adecuados, sino más bien ofrecer soluciones efectivas y específicas para cada tipo de enfermedad o patología humana. En este sentido, estrategias innovadoras como la ingeniería de tejidos o la medicina regenerativa, los sistemas de liberación controlada de fármacos y las nanomedicinas, surgen como buenas alternativas para abordar situaciones difíciles de resolver aplicando los tratamientos y estrategias terapéuticas convencionales, como es el caso cuando se hace necesario reemplazar tejidos o incluso órganos dañados por algún traumatismo o enfermedad. Concretamente, el presente trabajo de investigación tiene por objetivo principal diseñar un sistema combinado para la liberación controlada, estable y localizada de agentes terapéuticos que sean capaces de ejercer su efecto de forma selectiva sobre la zona que amerita el tratamiento. Este constructo tendrá la versatilidad suficiente como para poder adaptarse a casi cualquier tipo de tratamiento, desde el cáncer hasta la regeneración de tejido, siempre que el requisito clave del tratamiento sea la necesidad de suministrar el tratamiento de manera localizada, estable y controlada. Para efectos de facilitar la compresión y el diseño del sistema se escogió para la prueba de concepto materiales y fármacos asociados a la regeneración de tejidos, como tratamiento para casos de heridas crónicas. El sistema en cuestión está constituido por tres elementos principales: 1) El primer elemento son los conjugados poliméricos de agentes terapéuticos que contribuirán a aumentar la selectividad de la acción terapéutica del fármaco, así como también a mejora la estabilidad, biodisponibilidad y biocompatibilidad de los mismos. En caso de que el fármaco sea hidrofóbico, la conjugación contribuye a aumentar su solubilidad en agua, y en el caso de usar proteínas como agentes terapéuticos, la conjugación contribuye a disminuir la respuesta inmunológica del cuerpo incrementando las posibilidad de éxito del tratamiento. 2) El segundo elemento son micropartículas poliméricas biodegradables, que en este caso actúan con agentes de encapsulación para los conjugados poliméricos, permitiendo así contar con un segundo punto de control en la cinética de liberación de los agentes terapéuticos. Simultáneamente, las micropartículas también cumplen un papel de modificador de la textura del constructo final, adjudicándole propiedades mecánica y fisicoquímicas que contribuyen a mejorar las propiedades biológicas del material final, como son la afinidad, la adhesión y la proliferación celular. 3) El tercer elemento consiste en una membrana polimérica biodegradable nanoporosa hecha por electrospinning, que constituyen el elemento unificados del sistema, aporta manejabilidad al constructo y es en sí mismo el último punto de control en la cinética de liberación del agente terapéutico. Este último debe ser biocompatible y estable en condiciones ambientales, puesto que probablemente este expuesto al ambiente mientras protege la herida, en el caso concreto de este tipo de aplicación. Estos tres elementos, que en sí mismos constituyen sistemas complejos por separado, se han combinado sistemáticamente para alcanzar una relación sinérgica entre ellos de manera que cada uno potencia las cualidades de los otros dos. El constructo resultante se caracterizó demostrando tener propiedades características que se pueden utilizar como parámetro de control durante la fabricación del mismo. Así mismo estudios in vitro del sistema desarrollado señalan que puede ser un buen candidato para el tratamiento de heridas crónicas entre otras patologías que requieran tratamientos localizados. / [CA] Actualment, una de les majors preocupacions que permanentment llepen l'atenció dels principals sectors de la societat humana és la salut. La ciència mèdica moderna està compromesa no solament amb subministrar tractaments adequats, sinó més aviat oferir solucions efectives i específiques per a cada tipus de malaltia o patologia humana. En aquest sentit, estratègies innovadores com l'enginyeria de teixits o la medicina regenerativa, els sistemes d'alliberament controlat de fàrmacs i les nanomedicines, sorgeixen com a bones alternatives per a abordar situacions difícils de resoldre aplicant els tractaments i estratègies terapèutiques convencionals, com és el cas quan es fa necessari reemplaçar teixits o fins i tot òrgans danyats per algun traumatisme o malaltia. Concretament, el present treball de recerca té per objectiu principal dissenyar un sistema combinat per a l'alliberament controlat, estable i localitzada d'agents terapèutics que seguen capaços d'exercir el seu efecte de forma selectiva sobre la zona que amirita el tractament. Aquest constructe tindrà la versatilitat suficient com per a poder adaptar-se a quasi qualsevol tipus de tractament, des del càncer fins a la regeneració de teixit, sempre que el requisit clau del tractament sega la necessitat de subministrar el tractament de manera localitzada, estable i controlada. Per a efectes de facilitar la compressió i el disseny del sistema es va escollir per a la prova de concepte materials i fàrmacs associats a la regeneració de teixits, com a tractament per a casos de ferides cròniques. El sistema en qüestió està constituït per tres elements principals: 1) El primer element són els conjugats polimèrics d'agents terapèutics que contribuiran a augmentar la selectivitat de l'acció terapèutica del fàrmac, així com també a millora l'estabilitat, biodisponibilitat i biocompatibilitat dels mateixos. En cas que el fàrmac sega hidrofòbic, la conjugació contribueix a augmentar la seua solubilitat en aigua, i en el cas d'usar proteïnes com a agents terapèutics, la conjugació contribueix a disminuir la resposta immunològica del cos incrementant les possibilitat d'èxit del tractament. 2) El segon element són microparticles polimèriques biodegradables, que en aquest cas actuen amb agents d'encapsulació per als conjugats polimèrics, permetent així comptar amb un segon punt de control en la cinètica d'alliberament de l'agent terapèutics. Simultàniament, les microparticles també compleixen un paper de texturitzant del constructe final, adjudicant-li propietats mecànica i fisicoquímiques que contribueixen a millorar la propietats biològiques del material final, com són l'afinitat, l'adhesió i la proliferació cel·lular. 3) El tercer element consisteix en una membrana polimèrica biodegradable nanoporosa feta per electrospinning, que constitueixen el element unificats del sistema, aporta manejabilitat al constructe i és en si mateix el ultimi punt de control en la cinètica d'alliberament de l'agent terapèutic. Aquest últim ha de ser biocompatible i estable en condicions ambientals, ja que probablement aquest exposat a l'ambient mentre protegeix la ferida, en el cas concret d'aquest tipus d'aplicació. Aquests tres elements que en si mateixos constitueixen sistemes complexos per separat, s'han combinat sistemàticament per a aconseguir una relació sinergètica entre ells de manera que cadascun potencia les qualitats dels altres dos. El constructe resultant es va caracteritzar demostrant tenir propietats característiques que es poden utilitzar com a paràmetre de control durant la fabricació del mateix. Així mateix estudis in vitro del sistema desenvolupat assenyalen que pot ser un bon candidat per al tractament de ferides cròniques entre altres patologies que requeriren tractaments localitzats. / Rodríguez Escalona, GDJ. (2016). DEVELOPMENT OF CONTROLLED DRUG DELIVERY SYSTEMS OF POLYMERIC NANOMEDICINES ASSOCIATED TO SCAFFOLDS FOR TISSUE REGENERATION [Tesis doctoral]. Universitat Politècnica de València. https://doi.org/10.4995/Thesis/10251/63231

Ingeniería de tejidos

Polímeros terapéuticos

Administración localizada

Ácido hyalurónico

Enginyeria de teixits

Curcumina

Polímers terapèutics

Administració localitzada

Àcid hyalurònic

Tissue Engineering

Electrospinning-microparticle composite

Curcumin

PLLA

HA

MAQUINAS Y MOTORES TERMICOS