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首页> 外文期刊>EMBO Molecular Medicine >Absence of Runx3 expression in normal gastrointestinal epithelium calls into question its tumour suppressor function
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Absence of Runx3 expression in normal gastrointestinal epithelium calls into question its tumour suppressor function

机译:正常胃肠道上皮细胞中Runx3表达的缺乏质疑其抑癌功能

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The Runx3 transcription factor regulates cell fate decisions during embryonic development and in adults. It was previously reported that Runx3 is strongly expressed in embryonic and adult gastrointestinal tract (GIT) epithelium (Ep) and that its loss causes gastric cancer. More than 280 publications have based their research on these findings and concluded that Runx3 is indeed a tumour suppressor (TS). In stark contrast, using various measures, we found that Runx3 expression is undetectable in GIT Ep. Employing a variety of biochemical and genetic techniques, including analysis of Runx3?¢????GFP and R26LacZ/Runx3 Cre or R26tdTomato/Runx3 Cre reporter strains, we readily detected Runx3 in GIT?¢????embedded leukocytes, dorsal root ganglia, skeletal elements and hair follicles. However, none of these approaches revealed detectable Runx3 levels in GIT Ep. Moreover, our analysis of the original Runx3 LacZ/LacZ mice used in the previously reported study failed to reproduce the GIT expression of Runx3. The lack of evidence for Runx3 expression in normal GIT Ep creates a serious challenge to the published data and undermines the notion that Runx3 is a TS involved in cancer pathogenesis.
机译:Runx3转录因子在胚胎发育过程中和成年期调节细胞命运的决定。以前有报道说Runx3在胚胎和成年胃肠道(GIT)上皮(Ep)中强烈表达,其丢失会引起胃癌。已有280多家出版物基于这些发现进行了研究,并得出结论Runx3确实是一种抑癌剂(TS)。与之形成鲜明对比的是,我们使用各种措施发现在GIT Ep中无法检测到Runx3表达。利用多种生化和遗传技术,包括对Runx3αGFP和R26LacZ / Runx3 Cre或R26tdTomato / Runx3 Cre报告基因菌株的分析,我们很容易在嵌入GIT的白细胞,背根中检测到Runx3。神经节,骨骼元素和毛囊。但是,这些方法均未显示GIT Ep中可检测到的Runx3水平。此外,我们对先前报道的研究中使用的原始Runx3 LacZ / LacZ小鼠的分析未能重现Runx3的GIT表达。正常GIT Ep中Runx3表达的证据不足,对已发表的数据提出了严峻挑战,并破坏了Runx3是涉及癌症发病机制的TS的观念。

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