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  • About
  • The Global ETD Search service is a free service for researchers to find electronic theses and dissertations. This service is provided by the Networked Digital Library of Theses and Dissertations.
    Our metadata is collected from universities around the world. If you manage a university/consortium/country archive and want to be added, details can be found on the NDLTD website.
161

THE ROLE OF E-CADHERIN FORCE IN THE MAINTENANCE OF HOMEOSTASIS IN EPITHELIAL ACINI

Vani Narayanan, FNU 01 January 2016 (has links)
Numerous three-dimensional model systems have emerged for emulating the biochemical and physiological states of native tissue. Yet little is known about the effects of mechanical forces on cell behavior in the context of an organized tissue structure in three-dimensional cell-culture. Epithelial cells cultured in a three-dimensional environment comprised of extracellular matrix proteins form spheroids of polarized cells. Cellular responses to mechanical cues, generated from dynamic interactions with the extracellular matrix and neighboring cells, are known to influence cellular behavior to a great extent. Previous studies have shown that tumorigenic progression has been frequently linked to the down regulation of E-cadherin, a cell-cell adhesion protein. This work proposes that E-cadherin plays a pivotal role in maintaining epithelial tissue integrity and homeostasis. Novel FRET-based biosensors were used to measure force across E-cadherin. First, I observed that 3D acini had significantly higher force than 2D monolayers. Next, I determined that low-force mutant phenotypes of E-cadherin resulted in impaired lumen formation. In order to examine the effects of E-cadherin force on the disruption of homeostasis, TGF-b was used to induce epithelial to mesenchymal transition (EMT). TGF-b resulted in a decrease in E-cadherin force, even at early time points prior to transcriptional changes. Forskolin, a known regulator of acini lumen size, was shown to increase E-cadherin force. Furthermore, forskolin was able to prevent TGF-b disruptions in acini homeostasis. Finally, I examined how changes in substrate stiffness, known to affect acini lumen structure, altered E-cadherin forces. Stiffer substrates (mediated by collagen doping of Matrigel) delivered higher E-cadherin forces while simultaneously including acinar luminal filling. It is possible that signaling through non-junction forces, due to changes in ECM proteins, may mediate loss of the lumen. Thus, the major conclusion of these studies is that higher E-cadherin force is required for the formation and maintenance of a single central lumen in epithelial acini. Lower junctional forces induced acinar luminal filling, possibly through disruption in the polarity and subsequent cellular reorganization. This work, thus, establishes the role of E-cadherin as a key regulator of tissue homeostasis.
162

Etude du maintien de l'adhérence dans les tissus prolifératifs / Study of Adhesion Maintenance During Cell Division in Epithelial Tissues.

Guillot, Charlene 26 August 2014 (has links)
Les tissus épithéliaux présentent deux caractéristiques majeures, ils sont robustes (rôle de barrière) mais également plastiques lors de la morphogénèse. L'homéostasie des tissus épithéliaux repose sur la régulation de la balance prolifération/mort cellulaire. Dans ma thèse, je décris tout d'abord, les mécanismes moléculaires permettant à la cellule épithéliale de se diviser tout en maintenant l'intégrité du tissu. J'ai ensuite altéré cette intégrité, en utilisant le système de génération de clônes mosaïques, afin de comprendre comment la cohésion du tissu est maintenue. Ce travail m'a alors permis de comprendre comment l'adhérence est modulée, puis restaurée, au cours de la division cellulaire. Ainsi, j'ai montré que l'intégrité des tissus est assurée par l'action concomitante des forces d'adhésion et des forces de tension. Enfin, mon travail apporte également des éléments clés pour l'étude de la perte d'adhérence des cellules tumorales responsable en partie, de la progression des tumeurs solides en métastases. / Tissue homeostasis relies on the tight regulation of cell proliferation and cell death. Epithelial tissues are robust tissues that support the structure of developing embryos and adult organs and are effective barriers that physically protect the organism against pathogens. In my thesis, I have first described the molecular mechanisms responsible for maintaining tissue integrity during epithelial cell division. I have then abrogated this integrity by inducing mosaic clones within tissues to understand how tissue cohesion is maintained. This work shows how the continuity of adhesive properties is ensured during cell division. It also reveals new key elements that result in loss of adhesion in tissues and thus may be responsible for the progession from solid cancer to metastasis.
163

Expressão de CK5 e vimentina/E-caderina nos diferentes subtipos de carcinomas ductais mamários / Expression of CK5 and vimentin/E-cadherin in different subtypes of invasive ductal carcinoma

Rapatoni, Liane 17 September 2013 (has links)
Introdução: Os marcadores moleculares têm sido utilizados para identificar subgrupos de tumores com comportamento clínico distinto, inclusive quanto ao padrão de recidiva. Objetivo: Caracterizar a expressão imunoistoquímica de vimentina (VIM) e E-caderina (CDH1) em carcinomas ductais invasivos (CDI) de mama e sua associação com a expressão de citoqueratina 5 (CK5), e características clínico-patológicas. Métodos: Microarranjos teciduais (TMA) foram construídos a partir de 82 amostras de CDI de mama. Imunoistoquímica (IHQ) foi realizada para determinar os receptores hormonais (RH; receptores de estrógeno e progesterona) e receptor do fator de crescimento epidérmico humano 2 (HER2), VIM, CDH1, CK5 e Ki-67. Os tumores foram classificados como luminal A (RH+, HER2-), luminal B (RH+, HER2+ ou Ki-67 alto), HER2 hiperexpresso (RH-, HER2+) e triplo negativo (TN; RH-, HER2-). Resultados: O fenótipo VIM+/CDH1-/low não foi observado nos tumores luminal A, B e HER2 hiperexpresso, enquanto que este fenótipo estava presente em 61,9% dos TN (p= 0,0001). A mediana de Ki-67 em tumores VIM+/CDH1-/low foi 13,6 (variação, 17,8-45,4), em comparação com 9,8 (variação de 4,1-38,1) nos não- VIM+/CDH1-/low (p= 0,0007). O acometimento linfonodal foi menos freqüente em pacientes com VIM+/CDH1-/low do que nos não- VIM+/CDH1-/low (23% X 61%, teste de 2, p = 0,01). A sobrevida livre de doença em 5 anos foi de 61,5% e 83,7% (teste de log-rank, p= 0,02) e a sobrevida global em 5 anos foi de 51,2% e 83,5% (teste de log-rank, p= 0,03) em pacientes com tumores com fenótipo VIM+/CDH1-/low e não VIM+/CDH1-/low, respectivamente. Conclusão: A expressão de VIM e CDH1 identificaram um subconjunto de CDI de mama com fenótipo mesenquimal com alto grau histológico e alto índice mitótico. / Introduction: Molecular markers have been used to identify subgroups of tumors with distinct clinical behavior, including recurrence pattern. Objective: To characterize the immunohistochemical expression of vimentin (VIM) and E-cadherin (CDH1) in invasive ductal carcinoma (IDC) of the breast and its association with cytokeratin 5 (CK5) expression and clinicopathological features. Methods: A tissue microarray was constructed from 82 IDC breast cancer specimens. Immunohistochemistry (IHC) was used to determine hormone receptor (HR; estrogen and progesterone receptors) status and human epidermal growth factor receptor 2 (HER2), VIM, CDH1, CK5, and Ki-67 expression. Tumors were classified as luminal A (HR+, HER2-), luminal B (HR+, HER2+ or high Ki-67), HER2 enriched (HR-, HER2+), and triple negative (TNBC; HR-, HER2-). Results: The VIM+/CDH1-/low phenotype was not observed in luminal A, luminal B and HER2 enriched tumors, whereas this phenotype was present in 61.9% of triple negative (TNBC) tumors (p = 0.0001). The median Ki-67 index in VIM+/CDH1-/low tumors was 13.6 (range, 17.8-45.4) compared with 9.8 (range, 4.1-38.1) in non-VIM+/CDH1-/low tumors (p= 0.0007). The presence of lymph node metastasis was less frequent in patients with VIM+/CDH1-/low tumors than in those with non-VIM+/CDH1-/low tumors (23% vs. 61%; 2 test, p= 0.01). The 5-years disease-free survival was 61.5% and 83.7% (log-rank test; p= 0.02) and the 5-year overall survival was 51.2% and 83.5% (log-rank test; p= 0.03) in patients with VIM+/CDH1-/low phenotype and non-VIM+/CDH1-/low phenotype tumors, respectively. Conclusion: The expression of VIM and CDH1 identified a subset of IDC breast cancer of the mesenchymal phenotype with high histological grade and high mitotic index.
164

De la caractérisation des Cellules Initiant le Cancer Colorectal vers un biomarqueur pronostique et de surveillance des sujets traités pour cancer colorectal / From characterization of colorectal cancer initiating cells to a prognostic biomarker and monotoring of patients treated for colorectal cancer

Christou, Niki 03 March 2017 (has links)
Le Cancer Colo Rectal (CCR) est la deuxième cause de mortalité par cancer dans le monde. Le risque de récidive après traitement curatif atteint 45% pour les stades 3. Une des hypothèses à l’heure actuelle pouvant expliciter le processus métastatique et les récidives est la présence en son sein de cellules « souches », pouvant « initier » le cancer. Notre réflexion s’inscrit dans la continuité des travaux réalisés au sein de notre Laboratoire, intitulés «Stratégies d’isolement et de caractérisation des cellules initiatrices de cancer colorectal», (Mélin et al, 2012). Dans une première partie, notre travail a porté sur l’analyse in vitro de la sensibilité des fractions enrichies en CIC aux différentes molécules de chimiothérapie les plus couramment utilisées en cancérologie colorectale.Puis, dans une deuxième partie, l’analyse des tumeurs obtenues après greffe a été faite ex ovo sur la Membrane Chorio-Allantoïdienne d’embryon de poulet (CAM), modèle facilement manipulable, peu onéreux et très rapide. Ce modèle étant naturellement immunodéprimé, il permet d’obtenir des informations concernant les phénomènes clés de la tumorigénèse et de la néoangiogénèse. Des analyses de la croissance tumorale, de l’histologie (prolifération, apoptose et vascularisation) et des analyses protéiques ont été menées en parallèle. De cette dernière étude, un marqueur particulier la E cadhérine, a été mis en évidence comme témoin indirect d’agressivité. En effet, au sein des tumeurs obtenues à partir de F1 HCT116, fraction himiosensible, l’expression de la E cadhérine est augmentée contrairement aux tumeurs obtenues à partir de F3 WiDr, fraction chimiorésistante, montrant une diminution d’expression de la E cadhérine.Ainsi, dans une troisième partie, sachant qu’un lien entre cellules initiant le cancer et E cadhérine a été mis en évidence, nous nous sommes focalisés sur son expression. Nous avons alors étudié son expression in vitro sur des cellules résistantes au 5 Fluorouracile. Puis, son expression a été étudiée ex vivo au sein de tissus et de sérums de patients opérés de cancer colorectal. / The ColoRectal Cancer (CCR) is the second leading cause of cancer mortality in the world. The risk of recurrence after curative treatment reaches 45% for stages 3. One of the hypotheses currently able to explain the metastatic process and the recurrences is the presence within it of "stem" cells, which can "initiate" the cancer. Our reflection is in line with the work carried out in our Laboratory, entitled "Strategies for the isolation and characterization of cells that initiate colorectal cancer" (Mélin et al, 2012).In the first part, our work focused on in vitro analysis of the sensitivity of fractions enriched in CIC to different chemotherapy molecules most commonly used in colorectal cancer (CRC). Then, in a second part, the analysis of the tumors obtained after transplantation was made ex ovo on Chicken Embryo Chorio-Allantoid Membrane (CAM), an easily manipulated model, inexpensive and very fast. This model provides information on the key phenomena of tumorigenesis and neoangiogenesis. Analyzes of tumor growth, histology (proliferation, apoptosis and vascularization) and protein analyzes were carried out in parallel. From this last study, a particular marker, E cadherin, was highlighted as an indirect link with witness of aggressiveness. Indeed, within the tumors obtained from F1 HCT116, the chemosensitive fraction, the expression of cadherin E was increased in contrast to the tumors obtained from F3 WiDr, chemoresistant fraction, showing a decrease in expression of E cadherin.Thus, in a third part, knowing that a link between cells initiating cancer and E cadherin was highlighted, we focused on its expression. We first studied its expression in vitro on 5 Fluorouracilresistant cells. Its expression was then studied ex vivo in tissues and sera of operated patients of CRC.
165

Rôle de la petite GTPase Rap1 dans les effets proangiogéniques de l’angiopoïétine-1 sur les cellules endothéliales

Gaonac'h-Lovejoy, Vanda 05 1900 (has links)
No description available.
166

Implication de la VE-cadhérine dans la plasticité endothéliale des tumeurs / Role of VE-cadherin in tumor endothelial plasticity

Le Guelte, Armelle 16 October 2012 (has links)
La barrière hémato-encéphalique (BHE) régule le transport des molécules et des cellules du compartiment sanguin vers le système nerveux central. Pour assurer cette fonction, l’endothélium microvasculaire cérébral bénéficie d’un système particulier d’enzymes, de pompes d’efflux et de jonctions cellulaires spécialisées, qui ensemble contrôlent scrupuleusement le passage des molécules plasmatiques et des cellules circulantes. La VE-cadhérine est une molécule d’adhérence qui occupe une position unique dans l’organisation des jonctions endothéliales et le maintien de l’intégrité vasculaire. Cependant, même si le rôle de la VE-cadhérine est décrit comme fondamental au cours du développement du réseau vasculaire, sa participation dans l’intégrité de la BHE nécessite d’être explorée plus en détail. Le glioblastome, la tumeur cérébrale la plus agressive et la plus létale, est associée à une vascularisation hautement perméable. En outre, ces tumeurs renferment une sous-population de cellules souches gliomateuses (CSG) dérivant d’une fraction de cellules transformées à caractère souche, qui joueraient un rôle dans l’initiation et la progression tumorales, ainsi que dans la résistance aux thérapies conventionnelles. Plus particulièrement, ces cellules ont été retrouvées in situ en interaction directe avec les cellules endothéliales cérébrales. Néanmoins, l’implication des CSG dans la plasticité des cellules endothéliales cérébrales, et notamment la perméabilité vasculaire, n’a pas été étudiée. Au sein de notre équipe, nous avons démontré que les CSG sécrètent la Sémaphorine 3A (S3A), une molécule de répulsion caractérisée par une activité antiangiogénique et pro-perméabilité. La S3A induit une augmentation de la phosphorylation et de l’internalisation de la VE-cadhérine, conduisant à une perte de la fonction de barrière des cellules endothéliales cérébrales. Au niveau moléculaire, nous avons montré que Src, une tyrosine kinase, et Set, un inhibiteur naturel de PP2A, coopèrent pour inhiber l’activité phosphatase de PP2A en réponse à la S3A. Plus particulièrement, PP2A interagit avec la VE-cadhérine bloquant sa phosphorylation, son internalisation et l’ouverture de la barrière endothéliale. PP2A confère ainsi une stabilité à la VE-cadhérine, qui serait perturbée par la S3A produite localement par les CSG. Ce mécanisme pourrait jouer un rôle clé dans les défauts des vaisseaux irriguant les glioblastomes, et d’une manière générale dans la perméabilité vasculaire tumorale. L’ensemble de ces résultats nous permet de mieux caractériser les mécanismes moléculaires mis en jeu au cours de l’angiogenèse tumorale et d’envisager à long terme des molécules à visée thérapeutique, en ciblant par exemple la voie de signalisation activée par la S3A / The blood brain barrier (BBB) regulates the transport of molecules and cells from blood into the central nervous system. This implies that the cerebral microvascular endothelium has developed a particular system of enzymes, efflux pumps and specialized cell junctions, which together carefully control the passage of plasma molecules and circulating cells. Vascular endothelial (VE)-cadherin is an adhesion molecule that occupies a unique position in the organization of endothelial junctions and the maintenance of vascular integrity. In particular, phosphorylation and internalization of VE-cadherin destabilizes cell-cell contacts and increases permeability. However, though VE-cadherin is fundamental in the development of the vascular network, its participation in the integrity of the BBB needs to be further explored. Glioblastoma is the most aggressive and the most lethal brain tumor, which is characterized by a highly leaky vasculature. Furthermore, these tumors contain a subpopulation of glioma stem cells (GSC), which derive from a fraction of transformed stem cells. GSCs play a role in the tumor initiation, progression and resistance to conventional therapies. Notably, these cells were found in direct interaction with cerebral endothelial cells in situ. However, the involvement of GSCs in the plasticity of cerebral endothelial cells, including vascular permeability, has not been studied. Our team has demonstrated that GSCs secrete semaphorin 3A (S3A), a repulsive molecule characterized by anti-angiogenic and pro-permeability activity. S3A increased phosphorylation and internalization of VE-cadherin in cerebral endothelial cells, leading to a loss of barrier integrity. At the molecular level, Src, a tyrosine kinase, and Set, a natural inhibitor of PP2A, cooperate to inhibit the phosphatase activity of PP2A, in response to S3A. Specifically, we demonstrated that PP2A interacts with VE-cadherin at the basal level. This interaction blocks VE-cadherin phosphorylation and internalization and thereby prevents opening of the endothelial barrier. Thus, PP2A stabilizes VE-cadherin, and we further showed that this complex could be disrupted by S3A produced by GSCs. This mechanism could play a key role in the dysfunctions of the vessels supplying glioblastoma, and in tumor vascular permeability in general
167

Imunoexpressão de caderinas e integrinas no desenvolvimento do epitélio cutâneo humano / Immunoexpression of cadherins and integrins in the development of human skin epithelium

Leonardo Kamibeppu 15 June 2011 (has links)
Introdução: Caderinas e integrinas são importantes para a manutenção da integridade tecidual e transdução de sinal durante o desenvolvimento da pele. A distribuição destas moléculas no desenvolvimento da pele humana foi investigada e associada com os marcadores de diferenciação, Citoqueratinas (CK) e involucrina (INV). Método: Usando a técnica de imunoistoquímica foram investigadas as proteínas E- e P- caderinas, integrinas beta- 1 e -4, CK 10, CK 14 e INV em fragmentos de pele de várias regiões corpóreas de 7 fetos humanos (semana gestacional de 4 a 24, todos pesando até 500 g). Resultados: Na fase inicial do desenvolvimento, integrinas beta-1 e -4 and E- and P- caderinas estavam presentes na membrana plasmática das células epiteliais em todos as camadas do epitélio. CK14 e CK10 foram observadas em todas as camadas epiteliais e a INV fracamente detectada em células da camada mais superficial. Em estágios mais avançados, integrinas foram detectadas em todas as camadas epiteliais, com expressão polarizada principalmente na camada basal. E- caderina foi detctada em todas as camadas, menos no estrato cornificado e a P- caderina foi observada em camadas mais profundas do epitélio. CK14 estava presente na camada basal, CK 10 no estrato suprabasal e a INV foi observada no estrato cornificado. Conclusão: Caderinas e integrinas são essenciais para o desenvolvimento da pele, sendo espacialmente e temporalmente regulados. Suas expressões são relatas com a expressão da maturação de marcadores da epiderme. / Introduction: Cadherins and integrins are important for maintenance of tissue integrity and in signal transduction during skin development. Distribution of these molecules in human skin development was investigated and associated with markers of differentiation, cytokeratins (CK) and involucrin (INV). Methods: Using immunohistochemistry expression of E- and P- cadherins, integrins beta-1 and -4, CK10, CK 14 and INV was assessed in skin fragments of 7 human fetuses (gestacional weeks ranged from 4 to 24, all weighing up to 500 g). Results: At initial phases of development, integrins beta-1 and -4 and E- and P- cadherins were present on epithelial cell membranes in all layers. CK 14 and CK 10 were expressed in all epithelial layers and INV weakly detected in the superficial layer. In more advanced stages, integrins were detected in all layers, but a marked polarized expression was seen in basal layer. E- cadherin was detected in all layers, but the cornified stratum and P- cadherin were observed in the lower layers. CK 14 was expressed in layer, CK 10 in suprabasal stratum and INV was observed in cornified layer. Conclusions: Cadherins and integrins are essential for skin development, being spatially and temporally regulated. Their expression is related with the expression of maturation markers of the epidermis.
168

Imunoexpressão de caderinas e integrinas no desenvolvimento do epitélio cutâneo humano / Immunoexpression of cadherins and integrins in the development of human skin epithelium

Kamibeppu, Leonardo 15 June 2011 (has links)
Introdução: Caderinas e integrinas são importantes para a manutenção da integridade tecidual e transdução de sinal durante o desenvolvimento da pele. A distribuição destas moléculas no desenvolvimento da pele humana foi investigada e associada com os marcadores de diferenciação, Citoqueratinas (CK) e involucrina (INV). Método: Usando a técnica de imunoistoquímica foram investigadas as proteínas E- e P- caderinas, integrinas beta- 1 e -4, CK 10, CK 14 e INV em fragmentos de pele de várias regiões corpóreas de 7 fetos humanos (semana gestacional de 4 a 24, todos pesando até 500 g). Resultados: Na fase inicial do desenvolvimento, integrinas beta-1 e -4 and E- and P- caderinas estavam presentes na membrana plasmática das células epiteliais em todos as camadas do epitélio. CK14 e CK10 foram observadas em todas as camadas epiteliais e a INV fracamente detectada em células da camada mais superficial. Em estágios mais avançados, integrinas foram detectadas em todas as camadas epiteliais, com expressão polarizada principalmente na camada basal. E- caderina foi detctada em todas as camadas, menos no estrato cornificado e a P- caderina foi observada em camadas mais profundas do epitélio. CK14 estava presente na camada basal, CK 10 no estrato suprabasal e a INV foi observada no estrato cornificado. Conclusão: Caderinas e integrinas são essenciais para o desenvolvimento da pele, sendo espacialmente e temporalmente regulados. Suas expressões são relatas com a expressão da maturação de marcadores da epiderme. / Introduction: Cadherins and integrins are important for maintenance of tissue integrity and in signal transduction during skin development. Distribution of these molecules in human skin development was investigated and associated with markers of differentiation, cytokeratins (CK) and involucrin (INV). Methods: Using immunohistochemistry expression of E- and P- cadherins, integrins beta-1 and -4, CK10, CK 14 and INV was assessed in skin fragments of 7 human fetuses (gestacional weeks ranged from 4 to 24, all weighing up to 500 g). Results: At initial phases of development, integrins beta-1 and -4 and E- and P- cadherins were present on epithelial cell membranes in all layers. CK 14 and CK 10 were expressed in all epithelial layers and INV weakly detected in the superficial layer. In more advanced stages, integrins were detected in all layers, but a marked polarized expression was seen in basal layer. E- cadherin was detected in all layers, but the cornified stratum and P- cadherin were observed in the lower layers. CK 14 was expressed in layer, CK 10 in suprabasal stratum and INV was observed in cornified layer. Conclusions: Cadherins and integrins are essential for skin development, being spatially and temporally regulated. Their expression is related with the expression of maturation markers of the epidermis.
169

Caractérisation des fonctions génomiques de variants du récepteur des androgènes dans le cancer de la prostate / Transcriptional activities of androgen receptor variants in prostate cancer

Ould Madi-Berthelemy, Pauline 25 September 2018 (has links)
Le récepteur des androgènes (RA) est la principale cible thérapeutique du cancer de la prostate (CaP) métastatique. Bien que cette thérapie soit initialement efficace, les effets sont transitoires. De nombreux mécanismes peuvent expliquer la progression du CaP vers un stade de résistance à la castration, telles les modifications du RA. Des données récentes ont montré que les variants constitutifs RA-Q641X et RA-V7, caractérisés par la perte du domaine de liaison au ligand, étaient associés à l’expression de marqueurs mésenchymateux. L’étude de la régulation de la N-cadhérine a mis en évidence que si le RA sauvage et les variants constitutifs se liaient tous deux aux éléments de réponse du gène codant, seuls les derniers étaient associés à une augmentation de l’acétylation de l’histone H4, marque positive de la transcription. Le RNA-seq a révélé que leur expression était aussi corrélée à la régulation de sets de gènes spécifiques incluant des facteurs de transcription dont certains ont déjà été caractérisés en cancérologie.En ce qui concerne le RA-T576A, porteur d’une mutation faux-sens, les données ont révélé une séquence consensus de liaison à l’ADN moins conservée pour le RA sauvage que pour ce mutant et l’importance du 11ème nucléotide des éléments de réponse. De plus, cette mutation a semblé impacter le transcriptome du RA. Ce travail met en évidence le comportement distinct des variants du RA et aide à mieux comprendre leurs modes d’action en décrivant leurs activités transcriptionnelles. / The androgen receptor (AR) is the main therapeutic target in metastatic prostate cancer (PCa). Although this therapy is initially effective, the effects are transient. Many mechanisms can explain PCa progression toward castration resistance including abnormalities in the AR. Recent data have shown that constitutive AR (e.g AR-Q641X and AR-V7), which have lost the ligand binding domain, were associated with the induction of mesenchymal marker expression. The study of N-cadherin regulation highlighted that while both constitutive AR and wild type AR bound to response elements located in the encoding gene, only the AR variants were associated with an increase of H4 acetylation, a positive transcription mark. RNA-seq revealed that their expression was also correlated to specific sets of genes regulation, including transcription factors and genes involved in migration, AR regulation, and therapeutic resistance.Concerning AR-T576A, which hold a missense mutation, data revealed a less conserved consensus sequence for the wild type AR than for this mutant and highlighted the importance of the 11th nucleotide of the response element for AR recruitment to DNA. Plus, this mutation seemed to impair AR transcriptome. This work highlights the distinct AR variants’ behavior and helps to understand their mode of action by depicting their transcriptional landscapes.
170

Regulatory Effects of TGF-β Superfamily Members on Normal and Neoplastic Thyroid Epithelial Cells

Franzén, Åsa January 2002 (has links)
<p>Thyroid growth and function is partly regulated by growth factors binding to receptors on the cell surface. In the present thesis, the transforming growth factor-β (TGF-β) superfamily members have been studied for their role in regulation of growth and differentiation of both normal and neoplastic thyroid epithelial cells.</p><p>TGF-β1 is a negative regulator of thyrocyte growth and function. However, the importance of other TGF-β superfamily members has not been fully investigated. TGF-β1, activin A, bone morphogenetic protein (BMP)-7 and their receptors were found to be expressed in porcine thyrocytes. In addition to TGF-β1, activin A was also found to be a negative regulator of thyroid growth and function, and both stimulated phosphorylation and nuclear translocation of Smad proteins. Furthermore, TGF-β1 and epidermal growth factor (EGF) demonstrated a synergistic negative effect on thyrocyte differentiation. Simultaneous addition of the two factors resulted in a loss of the transepithelial resistance and expression of the epithelial marker E-cadherin. This was followed by a transient expression of N-cadherin.</p><p>Despite the extremely malignant character of anaplastic thyroid carcinoma (ATC) tumor cells, established cell lines are still responsive to TGF-β1. A majority of the cell lines were also found to be growth inhibited by BMP-7. BMP-7 induced cell cycle arrest of the ATC cell line HTh 74 in a dose- and cell density-dependent manner. This was associated with upregulation of p21<sup>CIP1</sup> and p27<sup>KIP1</sup>, decreased cyclin-dependent kinase (Cdk) activity and hypophosphorylation of the retinoblastoma protein (pRb). TGF-β1, and to some extent also BMP-7, induced the expression of N-cadherin and matrix metalloproteinase (MMP)-2 and -9. Stimulation of HTh 74 cells with TGF-β1 increased the migration through a reconstituted basement membrane indicating an increased invasive phenotype of the cells.</p><p>Taken together, these data show that TGF-β superfamily members not only affect growth and function of normal thyroid follicle cells but may also, in combination with EGF, play a role in cell dedifferentiation. This study additionally suggests that the TGF-β superfamily members may be important for the invasive properties of ATC cells.</p>

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