首页> 外文期刊>Canadian Journal of Biotechnology >Functional Genomic investigation of Peroxisome Proliferator-Activated Receptor Gamma (PPARG) mediated transcription response in gastric cancer
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Functional Genomic investigation of Peroxisome Proliferator-Activated Receptor Gamma (PPARG) mediated transcription response in gastric cancer

机译:过氧化物酶体增殖物激活受体γ(PPARG)介导的胃癌转录反应的功能基因组学研究。

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Cancer is a complex and progressive multi-step disorder that results from the transformation of normal cells to malignant derivatives. Several oncogenic signaling pathways are involved in this transformation. PPARG (Peroxisome proliferator-activated receptor gamma) mediated transcription and signaling is involved in few cancers. We have investigated the PPARG in gastric tumors. The objective of the present study was to investigate the PPARG mediated transcriptional response in gastric tumors. Gene-set based and pathway focused gene-set enrichment analysis of available PPARG signatures in gastric tumor mRNA profiles shows that PPARG mediated transcription is highly activated in intestinal sub-type of gastric tumors. Further, we have derived the PPARG associated genes in gastric cancer and their expression was identified for the association with the better survival of the patients. Analysis of the PPARG associated genes reveals their involvement in mitotic cell cycle process, chromosome organization and nuclear division. Towards identifying the association with other oncogenic signaling process, E2F regulated genes were found associated with PPARG mediated transcription. The current results reveal the possible stratification of gastric tumors based on the PPARG gene expression and the possible development of PPARG targeted gastric cancer therapeutics. The identified PPARG regulated genes were identified to be targetable by pioglitazone and rosiglitazone. The identification of PPARG genes also in the normal stomach tissues reveal the possible involvement of these genes in the normal physiology of stomach and needs to be investigated.
机译:癌症是一种复杂且进行性的多步骤疾病,由正常细胞向恶性衍生物转化而引起。该转化涉及几种致癌信号途径。 PPARG(过氧化物酶体增殖物激活受体γ)介导的转录和信号传导与几种癌症有关。我们已经研究了胃肿瘤中的PPARG。本研究的目的是研究胃癌中PPARG介导的转录反应。在胃肿瘤mRNA谱中可用PPARG标记的基于基因集和途径集中的基因集富集分析表明,在胃肿瘤的肠亚型中,PPARG介导的转录被高度激活。此外,我们已经获得了胃癌中PPARG相关基因,并确定了它们的表达与患者更好的存活率相关。对PPARG相关基因的分析显示它们参与有丝分裂细胞周期过程,染色体组织和核分裂。为了确定与其他致癌信号传导过程的关联,发现E2F调控的基因与PPARG介导的转录相关。当前的结果揭示了基于PPARG基因表达的胃肿瘤的可能分层以及以PPARG为靶标的胃癌治疗剂的可能发展。鉴定出的PPARG调节基因可被吡格列酮和罗格列酮靶向。在正常胃组织中的PPARG基因的鉴定也揭示了这些基因可能参与了胃的正常生理,需要进行研究。

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