首页> 美国卫生研究院文献>Molecular and Cellular Biology >Peyers Patch M Cells Derived from Lgr5+ Stem Cells Require SpiB and Are Induced by RankL in Cultured Miniguts
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Peyers Patch M Cells Derived from Lgr5+ Stem Cells Require SpiB and Are Induced by RankL in Cultured Miniguts

机译:Lgr5 +干细胞衍生的Peyers Patch M细胞需要SpiB并由RankL在培养的 Miniguts中诱导

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摘要

Peyer's patches consist of domains of specialized intestinal epithelium overlying gut-associated lymphoid tissue (GALT). Luminal antigens reach the GALT by translocation through epithelial gatekeeper cells, the so-called M cells. We recently demonstrated that all epithelial cells required for the digestive functions of the intestine are generated from Lgr5-expressing stem cells. Here, we show that M cells also derive from these crypt-based Lgr5 stem cells. The Ets family transcription factor SpiB, known to control effector functions of bone marrow-derived immune cells, is specifically expressed in M cells. In SpiB−/− mice, M cells are entirely absent, which occurs in a cell-autonomous fashion. It has been shown that Tnfsf11 (RankL) can induce M cell development in vivo. We show that in intestinal organoid (“minigut”) cultures, stimulation with RankL induces SpiB expression within 24 h and expression of other M cell markers subsequently. We conclude that RankL-induced expression of SpiB is essential for Lgr5 stem cell-derived epithelial precursors to develop into M cells.
机译:淋巴集结由覆盖肠相关淋巴样组织(GALT)的专用肠上皮域组成。发光抗原通过上皮网守细胞(所谓的M细胞)易位而到达GALT。我们最近证明,肠的消化功能所需的所有上皮细胞均由表达Lgr5的干细胞产生。在这里,我们显示M细胞也源自这些基于隐窝的Lgr5干细胞。 Ets家族转录因子SpiB,已知可控制骨髓衍生免疫细胞的效应子功能,在M细胞中特异性表达。在SpiB -/-小鼠中,M细胞完全不存在,它以细胞自主方式发生。已经显示出Tnfsf11(RankL)可以在体内诱导M细胞发育。我们显示在肠道类器官(“ minigut”)文化中,用RankL刺激可在24小时内诱导SpiB表达,随后表达其他M细胞标记。我们得出结论,SpiB的RankL诱导表达对于Lgr5干细胞衍生的上皮前体发展为M细胞至关重要。

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