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Hepatocyte Nuclear Factor 4α a Key Factor for Homeostasis Cell Architecture and Barrier Function of the Adult Intestinal Epithelium

机译:肝细胞核因子4α成年肠道上皮的稳态细胞结构和屏障功能的关键因素

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摘要

Hepatocyte nuclear factor 4α (HNF-4α) is a transcription factor which is highly expressed in the intestinal epithelium from duodenum to colon and from crypt to villus. The homeostasis of this constantly renewing epithelium relies on an integrated control of proliferation, differentiation, and apoptosis, as well as on the functional architecture of the epithelial cells. In order to determine the consequences of HNF-4α loss in the adult intestinal epithelium, we used a tamoxifen-inducible Cre-loxP system to inactivate the Hnf-4a gene. In the intestines of adult mice, loss of HNF-4α led to an increased proliferation in crypts and to an increased expression of several genes controlled by the Wnt/β-catenin system. This control of the Wnt/β-catenin signaling pathway by HNF-4α was confirmed in vitro. Cell lineage was affected, as indicated by an increased number of goblet cells and an impairment of enterocyte and enteroendocrine cell maturation. In the absence of HNF-4α, cell-cell junctions were destabilized and paracellular intestinal permeability increased. Our results showed that HNF-4α modulates Wnt/β-catenin signaling and controls intestinal epithelium homeostasis, cell function, and cell architecture. This study indicates that HNF-4α regulates the intestinal balance between proliferation and differentiation, and we hypothesize that it might act as a tumor suppressor.
机译:肝细胞核因子4α(HNF-4α)是在十二指肠到结肠以及从隐窝到绒毛的肠上皮中高表达的转录因子。这种不断更新的上皮的稳态取决于对增殖,分化和凋亡的综合控制,以及上皮细胞的功能结构。为了确定HNF-4α丢失在成人肠上皮中的后果,我们使用了他莫昔芬诱导型Cre-loxP系统使Hnf-4a基因失活。在成年小鼠的肠道中,HNF-4α的缺失导致隐窝的增殖增加,并导致Wnt /β-catenin系统控制的几个基因的表达增加。体外证实了HNF-4α对Wnt /β-catenin信号通路的控制。细胞谱系受到影响,杯状细胞数量增加,肠上皮细胞和肠内分泌细胞成熟受损。在没有HNF-4α的情况下,细胞间连接不稳定,细胞旁肠通透性增加。我们的结果表明,HNF-4α调节Wnt /β-catenin信号传导并控制肠上皮的稳态,细胞功能和细胞结构。这项研究表明,HNF-4α调节着肠细胞在增殖和分化之间的平衡,我们推测它可能起到抑癌作用。

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