Development of a magnetic suspension system and its applications in nano-imprinting and nano-metrology

Kuo, Shih-Kang

06 August 2003

No description available.

Engineering, Mechanical

magnetic suspension

motion control

nano-metrology

nano-imprinting

system identification

disturbance observer

Silicone Hydrogels and their use as Ophthalmic Drug Delivery Systems

Guidi, Giuliano

10 1900

<p>Despite the long history of topical eye drops and their use in delivering therapeutic agents to the anterior of the eye, efficient sustained delivery continues to be an elusive goal. The robust and effective clearance mechanisms that the eye is endowed with are significant delivery challenges and result in short drug residence times and low ocular bioavailability. The work carried out in this thesis focused on developing, synthesizing and characterizing silicone hydrogels and evaluating their potential as drug eluting inserts for more effective delivery of ocular pharmaceuticals. The first strategy (Chapter 2) focused on incorporating a novel hydrogel additive, hyaluronic acid, to promote hydrogel-drug ionic interactions that can function to increase drug loading and subsequent release dosage. Hydrogels composed of a hydrophilic monomer, N,N-dimethlacrylamide (DMA) or 2-hydroxyethyl methacrylate (HEMA), and a hydrophobic monomer, methacryloxypropyltris(trimethylsiloxy)silane (TRIS), were used as model contact lenses. By combining ionic interactions with molecular imprinting techniques within a single hydrogel, it was shown that this can produce a compound effect on drug uptake and release. Although greater control over release dosage was achieved, there was limited capacity for these materials to delivery timolol for extended periods with drug release occurring rapidly over a period of 1-2 days. However, there were clear differences in the release duration from the p(DMA-<em>co</em>-TRIS) and p(HEMA-<em>co</em>-TRIS) hydrogel formulations. Therefore, the second study (Chapter 3) aimed to better understand the relationship between the hydrogel chemical composition and the resultant material properties on the drug release characteristics. A range of hydrogels were synthesized with varying hydrophilic and hydrophobic monomers, which were then characterized by their water content, transparency, optical haze and surface wettability. The previous generation materials were evolved by incorporating a modified siloxy methacrylate TRIS(OH), a methacrylated polydimethylsiloxane macromonomer (mPDMS) and a polymerizable silicone surfactant (ACR). The properties of the hydrogels were dramatically affected by the nature and relative contribution of hydrophobic and hydrophilic monomers. The release of dexamethasone (DEX), an anti-inflammatory medication, was shown to vary significantly depending on the hydrogel formulations; often displaying faster release in high water content materials and slow release in low water content hydrogels. The mechanism of diffusion for lipophilic DEX in these hydrogel systems appeared to be through the internal aqueous network channels within the bulk. Over the range of hydrogels formulations that were tested, the release from them varied from approximately seven days to greater than two weeks.</p> / Master of Applied Science (MASc)

contact lens

drug delivery

glaucoma

molecular imprinting

silicone hydrogel

polymer

Biomaterials

Biomaterials

Asortativní párování u člověka. / Assortative mating in humans.

Štěrbová, Zuzana

January 2019

Human mate choice is far from random. Assortative mating can be either positive (homogamy), when people prefer and choose partners with self-similar characteristics, or negative (heterogamy, complementarity), when people prefer self-dissimilar partners. Over one hundred years of research, it has been shown that people generally couple based on the principle of homogamy. This thesis seeks to address the following two goals. First, it critically reviews the current state of knowledge in positive assortative mating (in particular, empirical support, factors affecting homogamy, mechanisms of homogamy, relationship and genetic impact of homogamy, and methodological pitfalls of research). This section includes theoretical papers deal with further mechanisms of assortative mating (homogamy, imprinting-like effect, heterogamy, complementarity). Second, the thesis provides further test of assortative mating in 'ideal partners' (preferences) and actual partners, in the context of sex, sexual orientation (heterosexual and non-heterosexual), and population (Brazil and Czech Republic). Results of these studies show that the principle of homogamy is valid irrespective of sex and population. However, they find a stronger tendency for homogamy in actual partners among heterosexuals than in homosexuals, although...

Konzistence a vliv otců na výběr partnera u heterosexuálních žen / Consistency and paternal influence on human mate choice in heterosexual women

Taskovská, Kristýna

January 2018

People choose partners based on different characteristics, however it is not clear whether they systematically choose partners with specific characteristics. It is also not clear what modulates partner preferences. One of the factors are parents, however the question is, whether parents influence all types of relationships (e.g. one-night stand, marriage etc.). The main objective was to analyze the consistency of mate choice in physical characteristics in heterosexual women. Another objective was to test paternal influence on the mate choice, and whether this influence differs among partners with whom women have children and partners with whom they don't. Last objective was to test whether the similarity between father and current partner influences the relationship and sexual satisfaction of the respondent. In total 693 heterosexual women, aged 18-45, participated in the research (average age = 30,7; SE = 5,9) and provided physical characteristics (weight, height, attractiveness, masculinity, eye color, hair color, facial masculinity, facial hair, musculature, BMI, relative height, body hair and leg length) of their father, current partner (with whom they had/were expecting children) and long term ex-partners (with whom they had no children), they completed the standardized questionnaire s-EMBU...

Evolution de la composition génétique du tissu nourricier de la graine : Double fécondation, polysporie et empreinte parentale / Evolution of the genetic make-up of seed nutritives tissues

Cailleau, Aurélie

13 December 2010

Chez les plantes à graine, l'albumen est un tissu nourricier surprenant, puisqu'il résulte de la double fécondation, qui est la fécondation concomitante de l'oosphère d'une part, et de la cellule mère de l'albumen, la cellule centrale, d'autre part. Dans cette thèse, nous étudions les pressions de sélection qui déterminent l'évolution de l'albumen et pourraient expliquer l'évolution (1) de la double fécondation, (2) d'un doublement des contributions maternelles dans la cellule centrale, (3) de la polysporie, qui consiste en la participation de plusieurs produits de méiose à la formation du gamétophyte, et (4) de l'empreinte parentale, l'expression différentielle des allèles maternels et paternels.Ces innovations modifient l'hétérozygotie dans le tissu nourricier et par conséquent, ont le potentiel de changer l'hétérosis de la graine. Dans cette thèse, nous commençons par étudier comment les changements génétiques qui découlent de la double fécondation, du doublement des contributions maternelles, de la polysporie et de l'empreinte parentale modifient l'hétérosis, ce qui peut jouer en faveur ou en défaveur de leurs évolutions. Puis, nous faisons une revue des données disponibles dans la littérature pour tester si ces traits sont le résultat d'un conflit mâle-femelle sur l'allocation des ressources. Enfin, nous étudions de manière expérimentale les patrons de l'allocation des ressources chez le maïs, pour tester si les embryons sont en compétition pour les ressources, ce qui est une des conditions nécessaires pour qu'un conflit sur l'allocation des ressources ait lieu.Nos modèles théoriques nous permettent de décrire un conflit mâle-femelle sur l'exposition des allèles délétères dans les tissus pour lesquels l'expression des gènes est asymétrique. Ce conflit n'avait jamais été décrit auparavant, et ouvre de nouvelles perspectives pour la compréhension de l'évolution de l'expression génétique. L'analyse des données indique que les théories alternatives à la théorie du conflit sur l'allocation des ressources ont parfois un bon pouvoir explicatif, et méritent par conséquent d'être d'avantage explorées. Enfin, notre étude expérimentale sur le maïs montre que la compétition entre embryons est prédominante lors de l'allocation des ressources chez cette espèce, ce qui est concordant avec les prédictions de la théorie du conflit sur l'allocation. / In seed plants, the endosperm is a surprising nutritive tissue, because it results from double fertilization, an eccentricity which results from the parallel fertilization of the egg cell on the one hand, and of the mother cell of the endosperm, the central cell, on the other hand. In this thesis, we study the selective pressures which drive the evolution of the endosperm and may explain the evolution of (1) double fertilization, (2) a doubling of maternal contributions in the central cell, (3) polyspory, the participation of several meiotic products to the gametophyte and (4) imprinting, the differential expression of maternal and paternal alleles. These innovations modify heterozygosity in the endosperm and as a consequence, have the potential to change heterosis in the seed. In this thesis, we first investigate how genetic changes that result from double fertilization, doubling of maternal contribution, polyspory and imprinting modify heterosis, which may play in favour or against the evolution of these traits. Second, we review the available data to test whether these traits are the result of a male-female conflict over resource allocation. Finally, we study experimentally patterns of resource allocation in maize to assess whether embryos compete for resources, which is a necessary condition for the conflict over resource allocation to occur. Our theoretical models allow us to describe a male-female conflict over the exposition of deleterious alleles in tissues with asymmetrical gene expression. This conflict had never been described before and opens perspectives for understanding the evolution of gene expression. We conclude from our analysis of data that theories which are alternative to the conflict theory over resource allocation may have a better explanatory power and therefore deserve to be further explored. Finally, our experimental study in maize shows that competition between embryos drives resource allocation in this species, which is consistent with predictions of the conflict over resource allocation theory.

Ressources

Mutations délétères

Allocation

Conflits

Empreinte parentale

Double fécondation

Resources

Deleterious mutations

Allocation

Conflicts

Genomic imprinting

Double fertilization

Caractérisation de la plasticité épigénétique du gène Necdin/NECDIN impliqué dans le syndrome de Prader-Willi et de ses conséquences fonctionnelles sur le phenotype

Rieusset, Anne

16 September 2013

Le syndrome de Prader-Willi est une maladie génétique rare. Les gènes candidats au SPW, dont le gène Necdin, sont régulés par l'empreinte génomique parentale : seul l'allèle paternel de ces gènes est exprimé, l'allèle maternel étant silencieux. Notre équipe a généré un modèle murin pour lequel l'allèle paternel de Necdin a été désactivé (+m/-p) et qui présente des similarités phénotypiques avec les patients PW. Ce phénotype est plus drastique chez les animaux -/-. Nous avons alors émis l'hypothèse que l'allèle maternel puisse avoir un rôle fonctionnel dans la survie des souris (+m/-p). L'expression de l'allèle maternel de Necdin est présente dans le système nerveux des souris (+m/-p). Cette expression, bien que faible au niveau transcriptionnel, est suffisante pour produire la protéine Necdin, ce qui a des conséquences cellulaires et physiologiques qui in fine permettent une amélioration du phénotype. Cette perte de silence de l'allèle maternel est également détectée dans l'hypothalamus de patients PW. Ces résultats révèlent une plasticité épigénétique inattendue qui permet d'envisager des perspectives thérapeutiques. / The Prader-Willi Syndrome (PWS) is a rare genetic disorder. Several genes, including NECDIN gene, are involved in the PWS. These genes are regulated by the genomic imprinting mechanism: only the paternal allele of these genes is expressed, their maternal allele being silenced. Our team has generated a mouse model in which the paternal allele of the Necdin gene has been deactivated (+m/-p). This model presents phenotypical similarities with PWS patients. We observed that mortality affects more -/- pups than +m/-p mice. Therefore we venture the hypothesis of a functional role of the maternal allele in mutant mice survival. We showed an expression of this allele in the nervous system of +m/-p mice. Though transcriptionnally low, that is sufficient to produce the Necdin protein and provoke cellular as well as physiological consequences that actively improve the phenotype. Importantly, a specific expression of the maternal NECDIN allele is also detected in hypothalamic brain sections of PWS patients. These results reveal an unexpected epigenetic flexibility that allow to contemplate a therapeutic pharmacological prospect.

Necdin

Plasticité épigénétique

Emprunte génomique Parentale

Syndrome de Prader-Willi

Necdin

Epigenetic plasticity

Parental genomic imprinting

Prader-Willi syndrome

612

Etude des mécanismes de transmission de dérégulations épigénétiques : analyse de la transmission spermatique chez l'homme / Mechanisms involved in the transmission of epigenetic deregulation : analyses of transmission in human sperm

Bruno, Céline

20 December 2018

Les notions selon lesquelles l’exposition environnementale peut être mémorisée et puisse dans des conditions défavorables favoriser l’apparition d’épimutations soulèvent la question d’une possible transmission transgénérationnelle chez l’Homme lorsque les gamètes sont atteints.Afin de répondre à la question du risque de transmission de dérégulation épigénétique (épimutation) chez l’Homme, nous l’avons abordé selon deux axes. Le premier nous a permis d’évaluer le risque de transmission intergénérationnelle chez un patient présentant un syndrome de Silver-Russell (SRS) et nous avons pu démontrer pour la première fois l’efficience de la reprogrammation épigénétique chez l’Homme pour des régions soumises à empreinte : disparition du défaut de méthylation du locus H19/IGF2 causal dans les gamètes du patient ainsi qu’une absence de transmission à sa descendance. Le second nous a conduit à dépister la présence d’épimutations spermatiques à partir de deux modèles : 1/ de pères d’enfants atteints de pathologies liées à l’empreinte parentale et 2/ de patients atteints de cancer testiculaire. Dans les 2 cas, l’analyse par pyroséquençage de leurs spermatozoïdes n’a pas mis en évidence de défaut d’empreinte. Néanmoins, nous avons retrouvé une association entre oligozoospermie et défaut d’empreinte spermatique.Le principal défi des études à venir est d’identifier les mécanismes intervenant dans l’apparition de ces épimutations. Les principales pistes convergent vers les petits ARNs non codants ou certaines régions de l’ADN dont les marques épigénétiques pourraient (au moins partiellement) échapper aux contrôles mis en place lors des phases successives de reprogrammation épigénétique. / The notion that environmental exposure can be memorized and promote epimutation (defined as defects on DNA methylation) raises the question of possible epigenetic transgenerational transmission in humans. To address whether an epimutation could be transmitted in humans, we pursued two axes. First, the evaluation of intergenerational transmission in the family of a Silver-Russell patient has shown, for the first time, the efficiency of epigenetic reprogramming in humans, specifically on imprinted regions. Indeed, no imprinted defect on causal H19/IGF2 locus was detected in the patient’s spermatozoa or in the DNA of his daughter. The second axis was to assess the presence of sperm epimutations 1/ from fathers of children diagnosed with imprinted syndromes and 2/ from men presenting testicular seminoma. Pyrosequencing analyses on imprinted genes did not reveal any alteration of sperm DNA methylation, though we confirmed an association between oligozoospermia and sperm imprinting defects.The next step will be to identify the mechanisms involved in the origin of the sperm epimutation. The main hypotheses converge to small non-coding RNAs or certain DNA regions which escape to controls setting up (at least partially) at the time of epigenetic reprogramming.

Epigénétique

Spermatozoide

Pathologie liée à l'empreinte

Epimutation

Méthylation de l'ADN

Transmission transgénérationnelle

Epigenetics

Spermatozoa

Imprinting syndrome

Epimutation

DNA methylation

Intergenerational inheritance

616.6

Intrauterine Growth Restriction (IUGR) and imprinted gene expression in the placenta: Role of PLAGL1 and analysis of the 6q24.2 Region

Iglesias Platas, Isabel

05 March 2012

BACKGROUND: Fetal growth is a complex process which depends on nutrient and oxygen availability and transport from the mother to the fetus across the placenta. This involves hormones and growth factors as well as maternal and fetal genes. The failure of the fetus to reach his or her full potential for growth is called Intrauterine Growth Restriction (IUGR) and implies risks for adverse short‐ and long‐ term outcomes. Imprinted genes are a specific subset of genes that display, in mammals and flowering plants, monoallelic expression depending on the parental origin of the allele. The regulation of imprinted expression depends on epigenetic mechanisms, a subset of heritable marks that have the ability to regulate DNA functions without altering its sequence. Imprinted genes tend to cluster in the genome due to coordinated regulation through Imprinting Control Centers, usually in the form of Differentially Methylated Regions between the paternally and maternally inherited alleles. Studies in both animals and humans as well as imprinting syndromes have uncovered a role for this group of genes in prenatal growth. Two imprinted genes (PLAGL1 and HYMAI) have been described in the 6q24 locus. Genetic and epigenetic defects in this region relate to the Transient Neonatal Diabetes Mellitus 1 phenotype, including severe growth restriction. We aimed to study the involvement of this region in non‐syndromic IUGR. PARTICIPANTS AND METHODS: One hundred placental samples from a cohort of healthy term singletons, fetal tissues from fifty‐four first trimester terminations and one hundred placental samples from healthy and complicated pregnancies of different gestational ages were used to analyze the role of the 6q24 region in normal fetal growth and IUGR, respectively. Relevant clinical data was obtained after informed consent. The methylation status of the 6q24 CpG islands was studied by array technology and bisulfite sequencing in normal term placenta and in first trimester fetal tissues. Methylation levels in the PLAGL1 DMR in healthy and IUGR placentas were compared by pyrosequencing. Allelic origin of expression was assessed by heterozygous DNA/cDNA SNP analysis. Levels of expression of imprinted transcripts were analyzed by qRT‐PCR. RESULTS: PLAGL1 P1, HYMAI and two newly described PLAGL1 isoforms (P3 and P4) were the only transcripts subjected to genomic imprinting in the investigated 6q24 region. Correspondingly, the CpG island associated to the P1 promoter was the only differentially methylated region. There was no correlation between PLAGL1 expression in the placenta and fetal size in uneventful pregnancies. In placentas from IUGR gestations, expression of HYMAI was significantly higher than in those from normally grown fetuses. Levels of expression of PLAGL1 were lower in IUGR and correlated positively and significantly with the presence of IUGR in placentas from girls, but not boys. These changes in expression were not mediated by Loss of Imprinting or abnormalities in the levels of methylation of the promoter‐associated DMR, but possibly by a change in regulatory posttranscriptional mechanisms, as suggested by the loss of correlation of PLAGL1 P1 and HYMAI expression in IUGR. CONCLUSIONS: Imprinted expression in the 6q24 region is limited to the PLAGL1/HYMAI locus, maybe due to demarcation of this region by CTCF boundaries. Intrauterine Growth Restriction is associated to abnormalities in expression of PLAGL1 and HYMAI in the placenta, which are not due to LOI or methylation changes.

Creixement fetal

Crecimiento fetal

Fetal growth

Epigenetics

Epigenética

Epigenètica

Impronta (Genética)

Impronta (Genètica)

Imprinting (Genetics)

Ciències de la Salut

618

Design and fabrication of flexible piezo-microgenerator with broadband width

Liu, Tong-Xin

15 July 2009

In this study the relationship between the dynamic response of the flexible substrate and the power generation for energy harvesting system is proposed. High electro-mechanical transformation of piezoelectric materials, high efficient energy transfer of mechanical structure and controlled circuit make the piezoelectric generator a high performance. The devices of cantilevers with lump structures on the flexible substrate and piezoelectric film (ZnO) are designed. Then some individual layers of power generator are stocked in parallel to form a multi-layer system with a broad resonant band width. When the generator is operated in a wide frequency range vibration environment, the multi-layer piezoelectric films in the form of cantilever structures can induce current. First the finite element method for the piezoelectric cantilever beam is constructed by using ANSYS software. Both modal analysis and harmonic response analysis are performed to obtain the structural modal parameters and frequency response functions, respectively. Besides, the beam structure is modeled by 3D coupled field piezoelectric element. This research will apply Taguchi¡¦s method to design including variations of dimensions and material properties for energy harvesting system. The flexible substrate is polymeric film (PET). Imprinting process is applied to transfer the simulated geometric configuration onto a flexible substrate to obtain a maximum power output. The results show the single devices can improve efficiently by using lump structures on the flexible substrate, the generator could achieve maximum OCV of 2.25V which is 0.276£gW every centimeter squared when attached to a stable source of vibration. The multi-layer system can be used in 50~500Hz of low frequency environment. Furthermore, the output voltage (OCV) is upward when the flexible substrate with low Young¡¦s modulus.

imprinting lithography

energy harvesting system

robust design

Taguch

finite element methods

ZnO

modal/harmonic analysis

flexible substrate

broad band width

Effect of DNA methyltransferase 1 on transmission ratio distortion and epigenetic inheritance

Yang, Lanjian, 1976-

January 2008

Epigenetic modification of DNA plays an important role in gene regulation. During gametogenesis and early embryogenesis epigenetic states are reset to ensure embryonic-specific gene expression patterns after fertilization. However, certain genomic regions may resist epigenetic reprogramming. This may result in transgenerational epigenetic inheritance. Earlier, a grandparental origin dependent (GPO) transmission ratio distortion (TRD) of alleles in the distal region of mouse chromosome 12 had been found (Croteau et al ., 2002). The distorted region overlaps with the imprinted region of chromosome 12. The mechanism underlying this TRD is unknown, and we hypothesized that it was due to failure to reset imprints in the imprinted region in a proportion of germ cells. Such an imprint resetting failure would represent a particular case of transgenerational epigenetic inheritance. DNA (Cytosine-5) methyltransferase 1 (DNMT1) plays a key role in the maintenance of epigenetic states in mammalian genomes. To test the role of DNA methylation and DNMT1 in the genesis of TRD and its relationship to epigenetic inheritance we investigated the effect of Dnmt1 loss-of-function mutations using two mouse models: GPO (grandparental origin dependent)-TRD (transmission ratio distortion) and epigenetic inheritance at the agouti locus. Here, we report that Dnmt1 mutations have a modifying parental effect on the transmission of grandparental chromosome 12 alleles. However, the same Dnmt1 mutation did not affect the agouti coat color inheritance patterns in mice that inherited the Avy (agouti viable yellow) mutant allele from the father. Our results suggest that Dnmt1 is a trans-acting modifier of allelic transmission and support the role of epigenetic states in the genesis of TRD.

Crosses, Genetic.

Inheritance Patterns -- genetics.

Genomic Imprinting -- genetics.

Mice.

Mice, Inbred C57BL.