Global ETD Search

71	Cell adhesion proteins in different invasive patterns of colon carcinomas : a morphometric and molecular genetic study Hahn-Strömberg, Victoria January 2008 (has links) Colorectal carcinoma is the second most common type of cancer in both men and women in Sweden. Cancer of the colon and rectum are often considered together and their ten year survival rate is approximately 50 – 60 % depending on sex and location. Different histopathological characteristics of such cancers, including the complexity of growth, are of importance for prognosis. This thesis has compared different morphometric methods in order to achieve a quantitative and objective measurement of the invasive front of colon carcinoma. Since the growth pattern is dependent on the cell adhesiveness of different proteins we studied the distribution and localization of E-cadherin, Beta-catenin, Claudin 1,2,7 and Occludin as well as screened the genes for mutations. We found a perturbed protein expression of E-cadherin, Beta-catenin, Claudin 1,2,7 and Occludin in tumor sections compared to normal mucosa, but no relation to tumor volume or growth pattern could be seen. The tumor volume was found to be correlated to the growth pattern but not responsible to the perturbed protein expression. In the mutation screening we found a SNP in exon 13 the E-cadherin gene in the tumor, as well as in exon 2 of Claudin 1 and exon 4 of Claudin 7 in both tumor and normal mucosa. No correlation between mutations and growth pattern or tumor volume was found. In conclusion, this thesis shows that the computer image analysis with estimation of fractal dimension and number of free tumor cell clusters is superior to the semi quantitative visual grading of tumor invasive complexity. The aberrant expression of cell adhesion proteins in the tumor compared to normal mucosa as well as polymorphisms in the cell adhesion genes CLDN1 and CLDN7 in both tumor and normal mucosa can suggest that these aberrations are important in the tumorigenesis of colon carcinoma. colon carcinoma growth pattern tight junction Complexity Index cell adhesion E-cadherin Beta-catenin Occludin Claudin. Medicine Medicin
72	Lesões de isquemia arteriovenosa e reperfusão em jejuno de equinos: imunoistoquímica de proteínas de junção e histopatologia NASCIMENTO, Aline Machado Rapello do 31 December 2007 (has links) Made available in DSpace on 2014-07-29T14:46:49Z (GMT). No. of bitstreams: 1 Dissertacao Aline Machado Rapello do Nascimento.pdf: 1403008 bytes, checksum: d5736b2cde9e7188a689131927c1127c (MD5) Previous issue date: 2007-12-31 / To evaluate whether complete arteriovenous ischemia followed by reperfusion of mesenteric blood flow aggravates lesions involving small intestine of horses, β--catenin and occludin expressions were measured in jejune epithelia of seven equines, without definite breed. The animals had been submitted to aseptic ventral midline celiotomy and five jejune segments collected corresponding to a baseline segment, a five minutes segment subjected to ischemia, and three segments collected after being subjected to five, sixty and one hundred and twenty minutes of tecidual reperfusion, respectively. Experimentally induced lesions created by total arteriovenous occlusion followed by reperfusion were similar to naturally acquired lesions, as much in the period of ischemia as in the aggravation of the injuries observed during reperfusion. Changes that occur when ischemic intestine is reperfused are progressive, and include mucosal, submucosal, and serosal edema; polymorphonuclear and mononuclear cell infiltrates; and alterations in vascular patterns. Imunohistochemistry analyses have shown strong staining baseline segments for β-catenin in all animals and its progressive lack of staining during ischemia and reperfusion treatments. That indicates progressive lack of intercellular adherence. Similar results of specific decreases of total expression of Occludin, a tight junction protein, were observed. This protein is involved in regulating the movement of solutes in the paracellular pathway and also plays an important role in the maintenance of cell polarity. The reduction of expressions of both intercellular proteins measured directly demonstrates β-catenin injury due to progression of edema during ischemia and its aggravation during reperfusion and also shows an increase of the permeability of paracelular pathways and its related consequences to degradation of Ocludina. / Realizou-se o estudo da patogenia da lesão por isquemia arteriovenosa completa dos vasos mesentéricos e reperfusão jejunal em eqüinos por meio da avaliação da expressão das proteínas β-catenina e ocludina presentes neste epitélio, em sete eqüinos, sem raça definida. Os animais foram submetidos á celiotomia asséptica na linha alba e coleta de cinco segmentos jejunais correspondestes á um segmento controle, um segmento tratado com isquemia por cinco minutos, e três segmentos coletados durante o período de reperfusão tecidual aos cinco, sessenta e cento e vinte minutos, respectivamente. As lesões induzidas experimentalmente por oclusão arteriovenosa total seguida por reperfusão foram similares às lesões adquiridas naturalmente tanto no período de isquemia quanto no agravamento das lesões observado nos tempos de reperfusão. As mudanças que ocorrem quando um intestino isquêmico sofre reperfusão são progressivas e incluem edema de mucosa, submucosa e serosa, infiltração polimorfonuclear e mononuclear e alterações nos padrões vasculares. A análise imunoistoquímica revelou forte expressão da β- catenina em todos os animais e a sua progressiva perda da expressão quando submetidos à isquemia e reperfusão. Isso indica perda progressiva da adesividade intercelular. Resultados similares de redução do total da expressão da Ocludina, uma proteína de junção de oclusão, foram observados. Esta proteína está envolvida na regulação dos movimentos dos solutos na via paracelular e também desempenha um importante papel na manutenção da polaridade celular. A diminuição da expressão de ambas as proteínas intercelulares demonstra a lesão à β-catenina devido à progressão do edema durante isquemia e o agravamento durante a reperfusão tecidual e também mostra um aumento na permeabilidade da via paracelular e suas conseqüências relacionadas à degradação da Ocludina. Beta-catenina junção de aderência junção de oclusão ocludina Beta-catenin adherents junction junction of occlusion occludin CNPQ::CIENCIAS BIOLOGICAS
73	Perfil de expressão de genes da via Wnt/beta-catenina em timócitos e linfócitos T CD4+ de camundongos BALB/c / Gene expression profile of Wnt/beta-catenin pathway elements in thymocytes and CD4 + T lymphocytes of BALB/c mice. Taccyanna Mikulski Ali 27 August 2015 (has links) INTRODUÇÃO: A molécula HIG2 pode atuar como agonista da via Wnt/beta-catenina, pois se liga ao receptor Frizzled 10 e induz a expressão de genes da mesma. Dados recentes do nosso grupo mostraram expressão diferencial do gene HIG2 em células mononucleares do sangue periférico e em especial linfócitos T CD4+ naïve, mas não em células diferenciadas de memória em indivíduos sadios. Também observamos in vitro em linfócitos T CD4+ de indivíduos saudáveis que o peptídeo sintético HIG2 induziu a ativação da via Wnt/beta-catenina, produção de HIG2 e outros produtos da via, além da proliferação de células T CD4+ naïve sugerindo um papel do HIG2 na proliferação homeostática de linfócitos T CD4+. HIPÓTESE: Como as células T CD4+ naïve são diretamente exportadas pelo timo, os níveis aumentados de HIG2 neste tipo celular sejam decorrentes da ativação da via Wnt/?-catenina nos estágios tardios da diferenciação de timócitos. Portanto, as células T CD4+ naïve e timócitos simples positivos para CD4 (SP CD4) apresentariam perfil semelhante de expressão de HIG2 e genes da via Wnt/beta-catenina, incluindo receptores, fatores de transcrição, genes estruturais da via e alvos quando comparadas as demais populações celulares. OBJETIVO: Avaliar a expressão de HIG2 e outros genes da via Wnt/beta-catenina em timócitos e linfócitos T CD4+ naïve e memória de camundongos. MÉTODOS: Isolamos timócitos duplo negativos (DN), timócitos duplo positivos (DP), simples positivos para CD4 e CD8 (SP CD4 e SP CD8) de timo e também células T CD4+ naïve e memória do baço dos mesmos camundongos pelo procedimento de citometria de fluxo. Analisamos a expressão de vários genes da via Wnt/beta-catenina por PCR em tempo real. RESULTADOS: Em timócitos DN há expressão significativa dos genes que codificam para Frizzled 6, LRP5, TCF-1 e TCF-4 em relação as outras populações celulares. Nos timócitos DP há maior expressão dos genes que codificam para LRP5, LRP6, beta-catenina, GSK-3beta, TCF-1 e Bcl-XL em relação às demais populações. Em timócitos SP CD4 foi detectada expressão diferencial de genes que codificam para Frizzled 10, LRP6, beta-catenina, LEF-1 e HIG2 enquanto que na população de timócitos SP CD8 não observamos expressão significativa de nenhum gene da via Wnt/beta-catenina. Nas células T CD4+ naïve há expressão significativa de Frizzled 5 e Frizzled 10 quando comparadas a timócitos SP CD8 e células T CD4+ de memória . Já nos linfócitos T CD4+ de memória, detectamos maior expressão de Frizzled 6, TCF-4, Bcl-XL e ciclina D1 em relação as demais populações. CONCLUSÃO: Cada população apresenta um perfil distinto de expressão gênica. As maiores semelhanças ocorrem entre os timócitos DN e DP onde as principais diferenças são a expressão de Frizzled 6 e Ciclina D1.Os timócitos SP CD4 e as células T CD4+ naïve não apresentaram níveis semelhantes de expressão gênica de elementos da via Wnt canônica, o que não corrobora a hipótese de que o perfil transcripcional de timócitos SP CD4 e linfócitos T CD4+ naïve é semelhante. Ainda, não observamos expressão aumentada de HIG2 em linfócitos T CD4+ naïve comparados aos de memória, o que contrasta com os resultados obtidos anteriormente por nosso grupo com amostras humanas sugerindo que camundongos não regulam a expressão de HIG2 em linfócitos T CD4+ como os seres humanos / INTRODUCTION: HIG2 molecule can act as an agonist of Wnt/?-catenin pathway, because it able to bind to Frizzled 10 receptor and induce the expression of the genes related to this pathway. Recent data from our group have shown differential expression of the HIG2 gene in peripheral blood mononuclear cells, and particularly in naive CD4 + T cells, but not in memory T cells in healthy individuals. We have also observed that inducing the CD4 + T lymphocytes from healthy individuals with HIG2 synthetic peptide in vitro, led to the activation of Wnt/beta-catenin pathway, HIG2 production and expression of other target genes of this pathway and the proliferation of naïve CD4 + T cells, suggesting that HIG2 may play a role in homeostatic proliferation of CD4+ T cells. HYPOTHESIS: As naïve CD4 + T cells are directly exported from the thymus, we have hypothesized that increased levels of HIG2 in this cell type is due to the activation of Wnt/beta-catenin pathway in the later stages of thymocyte differentiation. Therefore, naïve CD4 + T cells and CD4 single-positive thymocytes (CD4 SP) may share a similar pattern of gene expression of HIG2 and Wnt/beta-catenin genes (genes that encodes receptors and co-receptors, transcription factors, structural and target genes) when compared to other cell populations. AIM: our major aim is to evaluate the expression of HIG2 and other genes of the Wnt/beta-catenin in thymocytes, naïve CD4 + T lymphocytes and memory CD4+ T cells from mice. METHODS: We have isolated thymocytes double negative (DN) T cells, positive double positive (DP) T cells, CD4 and CD8 single-positive thymocytes (CD4 SP and CD8 SP) of thymus from BALB/c mice and we have also isolated naïve CD4 + T cells and memory CD4+ T cells of the spleen from the same mice we have used the thymus. We have analysed the expression of several genes of Wnt/beta-catenin by real time PCR RESULTS: In DN cells there was expression of the Frizzled 6, LRP5, TCF-1 and TCF-4 genes compared to other cell populations. In DP thymocytes it could be observed a greater expression of LRP5, LRP6, beta-catenin, GSK-3beta, TCF-1 and Bcl-XL genes compared to other populations. In CD4 SP thymocytes, it was detected differential expression of the Frizzled 10, LRP6, beta-catenin, LEF-1 HIG2 genes and in CD8 SP cells we could not observe significant expression of any gene of Wnt/?-catenin pathway. In naïve CD4 + T cells there was a significant expression of Frizzled5 and Frizzled 10 genes when compared to all the samples. In memory CD4 + T cells, we have detected higher expression of Frizzled 6, TCF-4, Bcl-XL and cyclin D1 genes than in any other populations. CONCLUSION: Each population has a distinct gene expression pattern. The biggest similarities occur between DN and DP thymocytes where the main differences are the expression of Frizzled 6 and cyclin D1.However, the pattern of gene expression in SP thymocytes is not similar to those presented by naïve CD4+ T cells. Moreover, we have not observed increased expression of HIG2 in naïve CD4 + lymphocytes compared to memory CD4+ T cells, which contrasts the results obtained previously by our group with human samples suggesting that mice might not regulate the HIG2 expression in CD4 + T lymphocytes as human beings do Células T CD4+ naive HIG2 Timócitos Via Wnt/beta-catenina HIG2 Naive CD4+ T cells Thymocytes Wnt/beta-catenin pathway
74	O papel da via proteica Wnt em carcinomas de laringe / The role of the Wnt protein pathway in laryngeal cancer Carlos Eduardo Molinari Nardi 02 March 2018 (has links) Introdução: O câncer de laringe é a segunda neoplasia maligna mais comum no segmento cervicofacial. As caderinas epiteliais (E-caderinas) em conjunto com cateninas formam o complexo E-caderina-catenina que atuam na adesão célula-célula. A perda dessa molécula pode levar à redução ou até mesmo ausência de expressão de E-caderina na membrana celular, acúmulo citoplasmático de beta-catenina e sua translocação para o núcleo, contribuindo para eventos carcinogênicos. Objetivo: Avaliar a expressão de E-caderina e beta-catenina em pacientes com tumor laríngeo precoce ou avançado e na presença ou ausência de metástase cervical. Métodos: Realizou-se estudo retrospectivo de 52 pacientes portadores de carcinoma epidermoide glótico ou supraglótico, tratados entre 1998 a 2011 e avaliados de acordo com o sítio de localização tumoral, grau de diferenciação histológica, estádio TNM, dados de sobrevida e confrontados com a expressão imunoistoquímica de E-caderina e beta-catenina. Resultados: Observou-se associação com significância estatística entre a queda da expressão de E-caderina com a localização supraglótica da lesão, a presença de metástase cervical, em tumores pouco diferenciados e em tumores localmente avançados quando em topografia glótica. Com relação à expressão de beta-catenina, também foi encontrada significância estatística ao relacionar a presença de metástase cervical e tumor de baixa diferenciação com a diminuição de expressão deste marcador. Quanto à análise de sobrevida, a baixa expressão de beta-catenina está relacionada a pior sobrevida global e a redução da expressão de ambos os marcadores a pior sobrevida livre de doença. Conclusão: A expressão anômala dos marcadores estudados levam a impacto prognóstico por poder propiciar tumores com maior agressividade local e presença de metástase cervical / Introduction: Larynx cancer is the second most common malignant neoplasm in the cervicofacial segment. Epithelial cadherins (E-cadherins) together with catenins form the E-cadherin-catenin complex that acts on cell-to-cell adhesion. The loss of this molecule may lead to the reduction or even absence of E-cadherin expression in the cell membrane, cytoplasmic accumulation of beta-catenin and its translocation to the nucleus, contributing to carcinogenic events. Objective: To evaluate the expression of E-cadherin and beta-catenin in patients with laryngeal tumor in different locoregional situations. Methods: A study retrospective of 52 patients with glottic or supraglottic squamous cell carcinoma treated between 1998 and 2011 was conducted, evaluated according to the tumor localization site, the degree of histological differentiation, TNM stage and survival analysis. These data were confronted with the immunohistochemical expression of E-cadherin and ?-catenin. Results: We observed statistically significant association between the fall of E-cadherin expression and the supraglottic localization of the lesion, the presence of cervical metastasis, poorly differentiated tumors and locally advanced tumors when in glottic topography. Related to the expression of beta-catenin, statistical significance was also found for the presence of cervical metastasis and tumor of low differentiation with the decreased expression of this marker. Regarding survival analysis, the low expression of beta-catenin is related to worse overall survival and the reduction of expression of both markers to worse disease-free survival. Conclusion: The anomalous expression of the markers studied leads to a prognostic impact in order to provide tumors with greater local aggressiveness and presence of cervical metastasis Beta catenina Caderinas Carcinoma Células escamosas Laringectomia Neoplasias laríngeas Beta catenin Cadherins Carcinoma Laryngeal neoplams Laryngectomy Squamous cell
75	Imunoexpressão da E-caderina, Beta-catenina e TP53 em câncer gástrico familial / Imunoexpression of E-cadherin, Beta-catenin and TP53 in familial gastric cancer Paula Balthazar Bambino 03 June 2009 (has links) Introdução: Agregação familial é observada em cerca de 10% dos casos de câncer e 1 a 3% é hereditário. O tipo difuso pode estar relacionado à agregação familial e a alterações genéticas no gene CDH1, que codifica a proteína E-caderina. Alterações na imunoexpressão de Beta-catenina e p53 também são observadas. Objetivos: Analisar a imunoexpressão da E-caderina, Beta-catenina e TP53 em adenocarcinomas gástricos de pacientes com câncer gástrico familial e comparar com os dados clinicopatológicos, além dos achados das alterações genéticas destes pacientes, estudadas previamente nesta Instituição. Casuística e Métodos: Vinte e seis casos de adenocarcinoma gástrico em blocos de parafina de pacientes do HC-FMUSP foram submetidos ao estudo imunoistoquímico para detecção e análise do padrão de imunoexpressão da E-caderina, Beta-catenina e TP53 através do método da streptavidina-biotina-peroxidase. A análise da imunoexpressão dos marcadores foi classificada segundo escala de intensidade e distribuição e os testes estatísticos utilizados foram o Teste t de Student e Exato de Fisher. Resultados: A localização predominante do tumor foi no antro (61,5%). 11 (42,3%) casos alterados para a imunoexpressão da E-caderina, sendo todos do tipo difuso; 15 (57,7%) casos normais, sendo 9 do tipo difuso e 6 do tipo intestinal (p=0,02). Em estudo prévio realizado nesta instituição, uma mutação missense no exon 12 do gene CDH1, códon 617, nucleotídeo 1849 G>A foi encontrada no mesmo caso em que foi observada ausência de imunorreatividade da E-caderina. 11 (42,3%) casos alterados para a imunoexpressão de Beta-catenina e 46,2% de imunorreatividade nuclear positiva para TP53. Conclusões: 1) O tipo difuso de Laurén está associado à alteração da imunoexpressão da E-caderina no Câncer Gástrico Familial; 2) Não houve associação entre a imunoexpressão da E-caderina, idade, gênero e localização do tumor; tampouco houve associação entre a imunoexpressão da Beta-catenina e os dados clínico-patológicos; houve associação inversa entre a imunoexpressão da E-caderina e TP53; 3) Nos casos em que foram detectadas alterações na imunoexpressão, parece haver duas rotas distintas de carcinogênese envolvidas no CGF. / Introduction: Familial clustering is observed in about 10% of the gastric cancer cases and 1-3% is hereditary. Diffuse type gastric cancer is related to genetic alterations in CDH1 gene, which translates the E-cadherin protein. The abnormal expression of E-cadherin is characterized by low expression of cytoplasmatic staining, or loss of membranous immunoreactivity. Aim: to analyze the immunoexpression of E-cadherin, Beta-catenin and TP53 in gastric adenocarcinomas in patients with Familial Gastric Cancer and compare with clinical-pathologic data, including the genetic alterations of these patients, found previously on this institution. Methods: 26 cases of paraffin-embedded gastric adenocarcinoma tissue of patients of Hospital das Clinicas - School of Medicine of University of Sao Paulo underwent immunostaining to detect the presence and to analyze the pattern of immunoexpression of E-cadherin, Beta-catenin and TP53 using Streptavidine-Biotine-Peroxidade technique. The immunoexpression evaluation was performed utilizing a semiquantitative scale for intensity and distribution. The statistical analysis was done through Students t test and Fishers Exact test. Results: E-cadherin immunoexpression was negative in 11 cases (42.3%), and all of them were diffuse type of Laurén. 15 cases (57.7%) were positive for E-cadherin, from which 9 were of the diffuse type and 6 of intestinal type (p=0.02). In previous study performed on this institution, one missense mutation in exon 12 of CDH1 gene, codon 617, nucleotide 1849 G>A was found on the same case that absence of E-cadherin immunostaining was observed. 61.5% of the tumors were located in the antrum. Beta-catenin immunoexpression was altered in 43.2% and TP53 nuclear immunoreactivity was positive in 46.2% of the tumors. TP53 was solely detected in 12 (46.2%) of the tumors, while E-cadherin was altered in 10/26 (38.5%) negative TP53 tumors, p=0.01. Conclusions: 1) Diffuse type of Laurén is associated to E-cadherin immunoexpression alteration in Familial Gastric Cancer; 2) There was no association between E-cadherin immunoexpression and age, gender or tumor location, as well as there was no association between Beta-catenin and the clinical-pathologic data; there was an inverse association between immunoexpression of TP53 and E-cadherin; 3) There may be two distinct carcinogenesis pathways on familial gastric cancer cases that imunoexpression alterations were detected. Beta-catenina Câncer gástrico familial E-caderina Imunoexpressão Neoplasia gástrica p53 Beta-catenin E-cadherin Familial gastric cancer Immunostaining p53 Stomach neoplasms
76	Contribution à l’étude du rôle et de la régulation de Fra-1 dans le cancer / Contribution to the study of Fra-1's role and regulation in cancer Milord, Sandrine 19 October 2011 (has links) Fra-1 appartient à la famille des facteurs de transcription AP-1. Son expression est particulièrement élevée dans les cellules de cancer du sein qui n'expriment pas le récepteur aux œstrogènes (RE-), c'est-à-dire les cellules les plus agressives. L'inhibition de Fra-1 dans ces cellules entraîne une diminution de la motilité, de l'invasion et de la prolifération, mais elle entraîne aussi de profonds changements de morphologie. Les cellules RE-, qui présentent un phénotype mésenchymateux s'arrondissent et établissent un plus grand nombre de contacts cellule-cellule après l'inhibition de Fra-1. Dans les cellules RE-, la β-caténine est localisée au noyau ou dans le cytoplasme, ce qui est un marqueur de mauvais pronostic. Au cours de cette thèse, j'ai montré que Fra-1 régule la localisation nucléaire de la β-caténine et ainsi régule son activité transcriptionelle en agissant très tardivement sur la voie Wnt. J'ai également mis en évidence une interaction physique directe entre Fra-1 et la β-caténine qui pourrait être responsable de cet effet. De plus, l'analyse de microarrays par RT-QPCR a révélé la régulation d'autres gènes comme la mœsine, la fibronectine et l'extracellular matrix protein 1, qui pourraient également jouer un rôle dans la régulation de l'agressivité tumorale par Fra-1. Par ailleurs, Fra-1 est une protéine instable et nous avons montré qu'elle est phosphorylée et stabilisée par PKCθ. Fra-1 est d'ailleurs nécessaire à l'effet de la kinase sur la motilité cellulaire. / Fra-1 is a member of the AP-1 transcription factor family. It is aberrantly expressed in breast cancer cells lacking Estrogen Receptor (ER-) expression, which are the most aggressive ones. Fra-1 inhibition in these cells leads to a decreased in motility, invasion and proliferation, but also to deep morphologic changes. ER- cells, which present a mesenchymal phenotype, become rounder and establish a greater number of cell-cell contacts after Fra-1 inhibition. In ER- cells, β-catenin is nuclear or cytoplasmic, which is considering as a poor prognosis marker. During this PhD, I demonstrate that Fra-1, which acts very downstream in the Wnt/β-catenin signaling pathway, regulates the nuclear localization of β-catenin leading to up-regulation transcriptional activity of β-catenin. I also found that Fra-1 directly interacts with β-catenin. In addition, RT-QPCR microarrays analysis has revealed the regulation of other genes such as mœsin, fibronectin and extracellular matrix protein 1, which might also take part in the tumoral aggressiveness regulated by Fra-1. Moreover, we show that Fra-1, which is an unstable protein, is phosphorylated and stabilized by PKCθ. Furthermore, Fra-1 is necessary to mediate the kinase effect on cell motility. Ap-1 Fra-1 Beta catenine PKC theta Invasion cellulaire Ap-1 Fra-1 Beta catenin PKC theta Cell invasion
77	Global Deletion of Sost Increases Intervertebral Disc Hydration But May Trigger Chondrogenesis Tori Morgan Kroon (8810045) 07 May 2020 (has links) Intervertebral discs (IVD) degenerate earlier than many other musculoskeletal tissues and will continue to degenerate with aging. IVD degeneration affects up to 80 percent of the adult population and is a major contributing factor to low back pain. Anti-sclerostin antibody is an FDA-approved treatment for osteoporosis in postmenopausal women at high-risk for fracture and, as a systemic stimulant of the Wnt/LRP5/b-Catenin signaling pathway, may impact the IVD. Stabilization of b-Catenin in the IVD increases Wnt signaling and is anabolic to the extracellular matrix (ECM), while deletion of b-catenin or LRP5 decreases Wnt signaling and is catabolic to the ECM. Here, we hypothesized that a reduction of Sost would stimulate ECM anabolism. Lumbar and caudal (tail) IVD and vertebrae of Sost KO and WT (wildtype) mice (n=8 each) were harvested at 16 weeks of age and tested by MRI, histology, immunohistochemistry, Western Blot, qPCR, and microCT. Compared to WT, Sost KO reduced sclerostin protein and Sost gene expression. Next, Sost KO increased the hydration of the IVD and the proteoglycan stain in the nucleus pulposus and decreased the expression of genes associated with IVD degeneration, e.g., heat shock proteins. However, deletion of Sost was compensated by less unphosphorylated (active) b-Catenin protein in the cell nucleus, upregulation of Wnt signaling inhibitors Dkk1 and sFRP4, and catabolic ECM gene expression. Consequently, notochordal and early chondrocyte-like cells (CLCs) were replaced by mature CLCs. Overall, Sost deletion increased hydration and proteoglycan protein content, but activated a compensatory suppression of Wnt signaling that may trigger chondrogenesis and may potentially be iatrogenic to the IVD in the long-term. Biomarkers Diseases Clinical Pharmacology and Therapeutics Biomechanical Engineering hydration heat shock proteins genetic animal model aggrecan wnt signaling beta catenin
78	The identification of protein-protein interactors of the Coxsackievirus and Adenovirus Receptor (CAR) and their impact on cell migration / Fok, Patrick Terrence. January 2008 (has links) No description available. Cell Adhesion. ras GTPase-Activating Proteins. Receptors, Virus -- physiology. Tubulin. Receptors, Cytoplasmic and Nuclear. Transcription Factors. Cell Movement. beta Catenin.
79	Understanding and Exploiting Wnt5a and GSK3 Signaling in Inflammatory Disease Bhatt, Pooja 07 June 2013 (has links) No description available. Biomedical Research Cellular Biology Molecular Biology Atherosclerosis Wnt5a Alzheimer's disease inflammation GSK3 cytokines beta catenin inflammatory diseases
80	Chromatin-associated functions of the APC tumor suppressor protein Hankey, William C., IV January 2016 (has links) No description available. Biomedical Research APC tumor suppressor colorectal cancer canonical WNT signaling chromatin transcription AP-1 transcription factor ChIP-seq beta-catenin

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