971 resultados para voie Wnt


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MicroRNAs (miRNAs) are single-stranded non-coding RNAs that negatively regulate target gene expression through mRNA cleavage or translational repression. There is mounting evidence that they play critical roles in heart disease. The expression of known miRNAs in the heart has been studied at length by microarray and quantitative PCR but it is becoming evident that microRNA isoforms (isomiRs) are potentially physiologically important. It is well known that left ventricular (patho)physiology is influenced by transmural heterogeneity of cardiomyocyte phenotype, and this likely reflects underlying heterogeneity of gene expression. Given the significant role of miRNAs in regulating gene expression, knowledge of how the miRNA profile varies across the ventricular wall will be crucial to better understand the mechanisms governing transmural physiological heterogeneity. To determinine miRNA/isomiR expression profiles in the rat heart we investigated tissue from different locations across the left ventricular wall using deep sequencing. We detected significant quantities of 145 known rat miRNAs and 68 potential novel orthologs of known miRNAs, in mature, mature* and isomiR formation. Many isomiRs were detected at a higher frequency than their canonical sequence in miRBase and have different predicted targets. The most common miR-133a isomiR was more effective at targeting a construct containing a sequence from the gelsolin gene than was canonical miR-133a, as determined by dual-fluorescence assay. We identified a novel rat miR-1 homolog from a second miR-1 gene; and a novel rat miRNA similar to miR-676. We also cloned and sequenced the rat miR-486 gene which is not in miRBase (v18). Signalling pathways predicted to be targeted by the most highly detected miRNAs include Ubiquitin-mediated Proteolysis, Mitogen-Activated Protein Kinase, Regulation of Actin Cytoskeleton, Wnt signalling, Calcium Signalling, Gap junctions and Arrhythmogenic Right Ventricular Cardiomyopathy. Most miRNAs are not expressed in a gradient across the ventricular wall, with exceptions including miR-10b, miR-21, miR-99b and miR-486.

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A downstream target of the Wnt pathway, neurone glial-related cell adhesion molecule (Nr-CAM) has recently been implicated in human cancer development. However, its role in colorectal cancer (CRC) pathobiology and clinical relevance remains unknown. In this study, we examined the clinical significance of Nr-CAM protein expression in a retrospective series of 428 CRCs using immunohistochemistry and tissue microarrays. Cox proportional hazards regression was used to calculate hazard ratios (HR) of mortality according to various clinicopathological features and molecular markers. All CRC samples were immunoreactive for Nr-CAM protein expression, compared to 10 / 245 (4%) matched normal tissue (P <0.0001). Of 428 CRC samples, 97 (23%) showed Nr-CAM overexpression, which was significantly associated with nodal (P = 0.012) and distant (P = 0.039) metastasis, but not with extent of local invasion or tumor size. Additionally, Nr-CAM overexpression was associated with vascular invasion (P = 0.0029), p53 expression (P = 0.036), and peritoneal metastasis at diagnosis (P = 0.013). In a multivariate model adjusted for other clinicopathological predictors of survival, Nr-CAM overexpression correlated with a significant increase in disease-specific (HR 1.66; 95% confidence interval 1.11-2.47; P = 0.014) and overall mortality (HR 1.57; 95% confidence interval 1.07-2.30; P = 0.023) in advanced but not early stage disease. Notably, 5-fluorouracil-based chemotherapy conferred significant survival benefit to patients with tumors negative for Nr-CAM overexpression but not to those with Nr-CAM overexpressed tumors. In conclusion, Nr-CAM protein expression is upregulated in CRC tissues. Nr-CAM overexpression is an independent marker of poor prognosis among advanced CRC patients, and is a possible predictive marker for non-beneficence to 5-fluorouracil- based chemotherapy.

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Using genome-wide data from 253,288 individuals, we identified 697 variants at genome-wide significance that together explained one-fifth of the heritability for adult height. By testing different numbers of variants in independent studies, we show that the most strongly associated 1/42,000, 1/43,700 and 1/49,500 SNPs explained 1/421%, 1/424% and 1/429% of phenotypic variance. Furthermore, all common variants together captured 60% of heritability. The 697 variants clustered in 423 loci were enriched for genes, pathways and tissue types known to be involved in growth and together implicated genes and pathways not highlighted in earlier efforts, such as signaling by fibroblast growth factors, WNT/I 2-catenin and chondroitin sulfate-related genes. We identified several genes and pathways not previously connected with human skeletal growth, including mTOR, osteoglycin and binding of hyaluronic acid. Our results indicate a genetic architecture for human height that is characterized by a very large but finite number (thousands) of causal variants.

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The small leucine-rich repeat proteoglycan (SLRPs) family of proteins currently consists of five classes, based on their structural composition and chromosomal location. As biologically active components of the extracellular matrix (ECM), SLRPs were known to bind to various collagens, having a role in regulating fibril assembly, organization and degradation. More recently, as a function of their diverse proteins cores and glycosaminoglycan side chains, SLRPs have been shown to be able to bind various cell surface receptors, growth factors, cytokines and other ECM components resulting in the ability to influence various cellular functions. Their involvement in several signaling pathways such as Wnt, transforming growth factor-β and epidermal growth factor receptor also highlights their role as matricellular proteins. SLRP family members are expressed during neural development and in adult neural tissues, including ocular tissues. This review focuses on describing SLRP family members involvement in neural development with a brief summary of their role in non-neural ocular tissues and in response to neural injury.

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The oncogenic role of WNT is well characterized. Wntless (WLS) (also known as GPR177, or Evi), a key modulator of WNT protein secretion, was recently found to be highly overexpressed in malignant astrocytomas. We hypothesized that this molecule may be aberrantly expressed in other cancers known to possess aberrant WNT signaling such as ovarian, gastric, and breast cancers. Immunohistochemical analysis using a TMA platform revealed WLS overexpression in a subset of ovarian, gastric, and breast tumors; this overexpression was associated with poorer clinical outcomes in gastric cancer (P=0.025). In addition, a strong correlation was observed between WLS expression and human epidermal growth factor receptor 2 (HER2) overexpression. Indeed, 100% of HER2-positive intestinal gastric carcinomas, 100% of HER2-positive serous ovarian carcinomas, and 64% of HER2-positive breast carcinomas coexpressed WLS protein. Although HER2 protein expression or gene amplification is an established predictive biomarker for trastuzumab response in breast and gastric cancers, a significant proportion of HER2-positive tumors display resistance to trastuzumab, which may be in part explainable by a possible mechanistic link between WLS and HER2.

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Aberrant activation of Wnts is common in human cancers, including prostate. Hypermethylation associated transcriptional silencing of Wnt antagonist genes SFRPs (Secreted Frizzled-Related Proteins) is a frequent oncogenic event. The significance of this is not known in prostate cancer. The objectives of our study were to (i) profile Wnt signaling related gene expression and (ii) investigate methylation of Wnt antagonist genes in prostate cancer. Using TaqMan Low Density Arrays, we identified 15 Wnt signaling related genes with significantly altered expression in prostate cancer; the majority of which were upregulated in tumors. Notably, histologically benign tissue from men with prostate cancer appeared more similar to tumor (r = 0.76) than to benign prostatic hyperplasia (BPH; r = 0.57, p < 0.001). Overall, the expression profile was highly similar between tumors of high (≥ 7) and low (≤ 6) Gleason scores. Pharmacological demethylation of PC-3 cells with 5-Aza-CdR reactivated 39 genes (≥ 2-fold); 40% of which inhibit Wnt signaling. Methylation frequencies in prostate cancer were 10% (2/20) (SFRP1), 64.86% (48/74) (SFRP2), 0% (0/20) (SFRP4) and 60% (12/20) (SFRP5). SFRP2 methylation was detected at significantly lower frequencies in high-grade prostatic intraepithelial neoplasia (HGPIN; 30%, (6/20), p = 0.0096), tumor adjacent benign areas (8.82%, (7/69), p < 0.0001) and BPH (11.43% (4/35), p < 0.0001). The quantitative level of SFRP2 methylation (normalized index of methylation) was also significantly higher in tumors (116) than in the other samples (HGPIN = 7.45, HB = 0.47, and BPH = 0.12). We show that SFRP2 hypermethylation is a common event in prostate cancer. SFRP2 methylation in combination with other epigenetic markers may be a useful biomarker of prostate cancer.

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BACKGROUND: Wnt signaling is thought to be important in prostate cancer, in part because proteins such as beta-catenin can also affect androgen receptor signaling. beta-Catenin forms a cell adhesion complex with E-cadherin raising the possibility that loss of expression or a change in beta-catenin distribution in the cell could also alter downstream signaling, decreased inter-cellular adhesion and the promotion of metastasis. A number of studies have reported the altered expression and/or localization of beta-catenin as a biomarker in prostate cancer.

METHODS: Tissue microarrays comprised of BPH and low, moderate and high-grade prostate cancer (n=77) were assessed for beta-catenin expression and distribution using immunohistochemistry. Staining was also performed on a tissue microarray containing tissue from patients before and after hormone manipulation. The effects of fixation and different antibodies was assessed on fixed LNCaP cell pellets and small prostate tissue microarrays.

RESULTS: We have observed increased beta-catenin expression in only high Gleason score (>7) prostate cancer. A nuclear re-distribution of beta-catenin has previously been reported. We noted nuclear beta-catenin in benign prostatic hyperplasia and a gradual loss in nuclear distribution with increasing Gleason grade. We found no evidence for an alteration in beta-catenin expression or re-distribution with hormone ablation. Altered fixation, antibodies and antibody concentration did affect the intensity and specificity of staining.

CONCLUSIONS: A loss of nuclear beta-catenin is the most consistent feature in prostate cancer rather than absolute levels of expression. We also suggest that variation in immunohistochemical protocols may explain variations in the reported literature.

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Aberrant activation of Wnt/β-catenin signaling, resulting in the expression of Wnt-regulated oncogenes, is recognized as a critical factor in the etiology of colorectal cancer. Occupancy of β-catenin at promoters of Wnt target genes drives transcription, but the mechanism of β-catenin action remains poorly understood. Here, we show that CARM1 (coactivator-associated arginine methyltransferase 1) interacts with β-catenin and positively modulates β-catenin-mediated gene expression. In colorectal cancer cells with constitutively high Wnt/β-catenin activity, depletion of CARM1 inhibits expression of endogenous Wnt/β-catenin target genes and suppresses clonal survival and anchorage-independent growth. We also identified a colorectal cancer cell line (RKO) with a low basal level of β-catenin, which is dramatically elevated by treatment with Wnt3a. Wnt3a also increased the expression of a subset of endogenous Wnt target genes, and CARM1 was required for the Wnt-induced expression of these target genes and the accompanying dimethylation of arginine 17 of histone H3. Depletion of β-catenin from RKO cells diminished the Wnt-induced occupancy of CARM1 on a Wnt target gene, indicating that CARM1 is recruited to Wnt target genes through its interaction with β-catenin and contributes to transcriptional activation by mediating events (including histone H3 methylation) that are downstream from the actions of β-catenin. Therefore, CARM1 is an important positive modulator of Wnt/β-catenin transcription and neoplastic transformation, and may thereby represent a novel target for therapeutic intervention in cancers involving aberrantly activated Wnt/β-catenin signaling.

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Bone Mineral Density (BMD) is a highly heritable trait, but genome-wide association studies have identified few genetic risk factors. Epidemiological studies suggest associations between BMD and several traits and diseases, but the nature of the suggestive comorbidity is still unknown. We used a novel genetic pleiotropy-informed conditional False Discovery Rate (FDR) method to identify single nucleotide polymorphisms (SNPs) associated with BMD by leveraging cardiovascular disease (CVD) associated disorders and metabolic traits. By conditioning on SNPs associated with the CVD-related phenotypes, type 1 diabetes, type 2 diabetes, systolic blood pressure, diastolic blood pressure, high density lipoprotein, low density lipoprotein, triglycerides and waist hip ratio, we identified 65 novel independent BMD loci (26 with femoral neck BMD and 47 with lumbar spine BMD) at conditional FDR < 0.01. Many of the loci were confirmed in genetic expression studies. Genes validated at the mRNA levels were characteristic for the osteoblast/osteocyte lineage, Wnt signaling pathway and bone metabolism. The results provide new insight into genetic mechanisms of variability in BMD, and a better understanding of the genetic underpinnings of clinical comorbidity.

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BACKGROUND: In spite of the recent discovery of genetic mutations in most myelodysplasic (MDS) patients, the pathophysiology of these disorders still remains poorly understood, and only few in vivo models are available to help unravel the disease.

METHODS: We performed global specific gene expression profiling and functional pathway analysis in purified Sca1+ cells of two MDS transgenic mouse models that mimic human high-risk MDS (HR-MDS) and acute myeloid leukemia (AML) post MDS, with NRASD12 and BCL2 transgenes under the control of different promoters MRP8NRASD12/tethBCL-2 or MRP8[NRASD12/hBCL-2], respectively.

RESULTS: Analysis of dysregulated genes that were unique to the diseased HR-MDS and AML post MDS mice and not their founder mice pointed first to pathways that had previously been reported in MDS patients, including DNA replication/damage/repair, cell cycle, apoptosis, immune responses, and canonical Wnt pathways, further validating these models at the gene expression level. Interestingly, pathways not previously reported in MDS were discovered. These included dysregulated genes of noncanonical Wnt pathways and energy and lipid metabolisms. These dysregulated genes were not only confirmed in a different independent set of BM and spleen Sca1+ cells from the MDS mice but also in MDS CD34+ BM patient samples.

CONCLUSIONS: These two MDS models may thus provide useful preclinical models to target pathways previously identified in MDS patients and to unravel novel pathways highlighted by this study.

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Acompanhando o crescente e recente interesse pela actividade do professor em sala de aula, esta investigação visa analisar, grosso modo, o papel assumido pelas ferramentas didácticas quer nas práticas docentes propriamente ditas quer no objecto efectivamente ensinado em sala de aula. Procuramos analisar, em síntese, de que forma a introdução de uma nova ferramenta de ensino – uma sequência didáctica – a mobilizar, in loco, pelo professor poderá gerar transformações não só nos próprios procedimentos de ensino do professor como também na própria forma como o objecto de ensino é (re)configurado no seio das interacções didácticas. Esta é, assim, a questãochave da nossa pesquisa, fundada em diferentes mas complementares correntes teóricas. De molde a procurar obter uma resposta a tal interrogação, desenhámos uma investigação em redor, concretamente, do ensino da escrita do texto de opinião, em turmas de sexto ano de escolaridade, que se desenrolou em duas grandes fases: i) numa primeira, cada professor ensina o objecto como lhe apraz; ii) numa segunda, cada professor procede, de novo, ao ensino desse objecto, mas, agora, com a nova ferramenta didáctica (a sequência didáctica) que a cada um é dada pela investigadora. A recolha dos dados efectuou-se mediante a gravação audiovisual das próprias aulas, realizando-se também entrevistas várias, com propósitos distintos, aos professores, antes e após cada uma das supracitadas fases. Os resultados demonstram a existência de uma série de transformações quer no plano das práticas dos professores quer no âmbito do objecto efectivamente ensinado. No entanto, foi também possível identificar aspectos vários em que a mudança não ocorreu ou, pelo menos, não foi significativa. Perante estes resultados, lançámo-nos ainda na formulação de determinadas perguntas, pistas para futuras investigações, cuja pertinência se nos afigura evidente, se se quiser reequacionar o papel das ferramentas didácticas no trabalho, em sala de aula, do professor.

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Cette recherche s'intéresse au parcours d'athlètes de haut niveau lors de leur transition d'une carrière sportive vers autre chose (nouvelle identité, nouvelle carrière, nouveaux projets, etc.). Même si les athlètes savent que la retraite sportive est la plupart du temps inévitable, plusieurs écrits soulignent les difficultés qui l'accompagnent, notamment sur le plan identitaire, les athlètes ayant à faire le deuil d'une identité fortement valorisée. Des retraités de la compétition sportive décrivent même cette étape comme le passage d'être exceptionnel à simple citoyen. Les écrits sur l'identité athlétique indiquent que le degré d'identification au rôle d'athlète et le degré d'exclusivité que la personne accorde à son rôle s'accroissent avec le niveau sportif atteint. La transition serait particulièrement difficile pour les athlètes de haut niveau, c'est-à-dire pour ceux qui ont obtenu une reconnaissance de leur statut d'athlète sous la forme d'une sélection pour des compétitions nationales ou internationales, dont les jeux olympiques. Lorsque ces personnes quittent la scène sportive, ils vivent un sentiment de vide et d'incertitude face à leur avenir. En plus d'avoir l'impression de perdre leur identité, ils disent manquer la stimulation, la reconnaissance sociale et le style de vie de leur ancienne vie. La transition serait particulièrement difficile pour les personnes qui partent à la retraite parce qu' elles y sont forcées, par exemple en raison de blessures. Les études qui ont utilisé une méthodologie qualitative ont permis de constater une évolution dans les questionnements identitaires des athlètes ainsi que sur la façon dont ils s'adaptent à leur nouvelle situation.Cette recherche poursuit dans cette voie en s'intéressant au parcours identitaire d'athlètes de haut niveau. Elle décrit les dynamiques et stratégies identitaires mises en oeuvre par des athlètes. Six athlètes de haut niveau ont été interrogés à propos de ce qu'ils ont vécu sur le plan identitaire durant leur carrière, mais principalement à partir du moment où celle-ci a pris fin. Les athlètes se sont également prononcés sur leurs projets d'avenir. Ces athlètes ont participé à la recherche sur une base volontaire, à la suite d'une invitation lancée par un organisme national de sport. Cet échantillonnage au hasard a mené à une grande diversité quant à la durée de la carrière (entre 15 et 25 ans de pratique sportive et 13 et 25 ans de participation à des compétitions), le nombre et l'ampleur des succès obtenus ainsi qu'au temps écoulé depuis leur retraite. Les données ont été analysées sous la forme d'études de cas, en faisant une mise en relation avec les composantes de l'identité athlétique (Cieslak, 2004), les dynamiques identitaires (Kaddouri, 1999, 2002, 2006) et les stratégies identitaires (Carver et al. , 2000). Même si tous les athlètes ont vécu une carrière marquée de succès importants, on observe une grande diversité dans la façon de réagir à la retraite. Certains s'engagent rapidement dans une dynamique de transformation identitaire, même avant la fin de la carrière, alors que d'autres passent par de nombreux tourments où se succède l'adoption de dynamiques identitaires différentes, axées parfois sur une redéfinition de l'identité ou une reconstruction de celle-ci. Les athlètes ont utilisé une grande diversité de stratégies pour s'adapter à leur nouvelle situation, parfois des stratégies de type résolution de problèmes par exemple en planifiant leur avenir avant de prendre leur retraite, parfois des stratégies de gestion des émotions, par exemple en réinterprétant la situation de façon positive ou en recherchant un soutien moral chez leurs proches. Certaines stratégies ont cependant été déclarées comme étant peu efficaces et les athlètes ont fourni quelques conseils pour les personnes qui font face à la transition de carrière sportive vers autre chose.

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Cet essai présente les résultats d'une recherche expérimentation en vue de valider un modèle de formation en ligne auprès des diététistes. Les besoins accrus de formation suscités par le nouveau cadre normatif amènent l'Ordre professionnel des diététistes du Québec (OPDQ) à développer différents moyens de perfectionnement pour ses membres. Bien que les moyens actuellement disponibles soient assez diversifiés, il importe de pouvoir offrir au plus grand nombre possible une offre de formation de haut niveau afin d'assurer e développement des compétences des diététistes. Comme l'OPDQ n'a pas les effectifs nécessaires pour former rapidement un grand nombre de personnes dispersées géographiquement, il devient intéressant d'explorer des moyens de formation complémentaires et d'envisager exploiter les possibilités offertes par la formation en ligne. C'est ainsi que l'auteure de cette recherche a constaté que l'ajout d'une offre complémentaire de formation en ligne pourrait grandement profiter aux diététistes afin de les aider à mieux répondre à l'obligation de mise à jour de leurs connaissances. Une enquête réalisée à l'été 2006 auprès des membres de l'OPDQ confirmait l'intérêt des répondantes pour ce type de formation ainsi que la présence des habiletés technologiques nécessaires. Les données alors recueillies ont permis de cibler une compétence à développer et d'expérimenter, auprès des diététistes, un modèle de formation en ligne portant sur le choix de la voie d'alimentation appropriée. Les objectifs spécifiques de la recherche expérimentation consistaient à élaborer un modèle de formation en ligne pour ensuite l'expérimenter auprès d'un groupe pilote de diététistes en exercice afin d'en évaluer le potentiel. Ce modèle identifiait les dimensions à considérer en ce qui concerne les apprenantes et les apprenants, leur accompagnement, le choix de la compétence et l'élaboration du système d'apprentissage.

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Le présent essai est l'aboutissement d'une réflexion sur la place qu'occupe le libre accès dans la communauté scientifique. Bien que le libre accès ne constitue pas en soi une nouveauté, il occupe une place relativement marginale. L'auteur s'est d'abord penché sur l'évolution du libre accès dans le monde avant d'entreprendre une recherche terrain a l'Université de Sherbrooke pour mesurer l'intérêt et les connaissances de la communauté de recherche. Au terme de cette recherche, l'auteur a produit une analyse à partir des données qu'il a récoltées. Des recommandations ont par la suite été produites à l'intention de la direction du Service des bibliothèques et archives (SBA) dans le but de promouvoir le libre accès, porteur selon l'auteur d'économies potentielles pour les universités et d'une plus grande accessibilité au savoir autant pour les chercheurs que pour le grand public. Voici un bref aperçu desdites recommandations: Recommandation 1: Mettre sur pied une séance d'information et une brochure présentant le libre accès aux professeurs et aux étudiants de l'Université de Sherbrooke. Recommandation 2: Encourager les facultés à faire en sorte que soient déposés sur Savoirs UdeS les articles publiés par les professeurs. Recommandation 3: Entamer un dialogue personnalise avec les représentants de l'ensemble des facultés de l'Université de Sherbrooke pour établir la voie verte au libre accès. Recommandation 4: Assurer la synergie des dépôts institutionnels des universités québécoises. Recommandation 5: Assurer la défense des intérêts universitaires par un réseautage auprès des organismes subventionnaires.