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应激传感器沿肠隐窝-绒毛轴的拓扑隔离。

Topological segregation of stress sensors along the gut crypt-villus axis.

作者信息

Touhara Kouki K, Rossen Nathan D, Deng Fei, Castro Joel, Harrington Andrea M, Chu Tifany, Garcia-Caraballo Sonia, Brizuela Mariana, O'Donnell Tracey, Xu Jinhao, Cil Onur, Brierley Stuart M, Li Yulong, Julius David

机构信息

Department of Physiology, University of California San Franscisco, San Francisco, CA, USA.

Tetrad Graduate Program, University of California San Francisco, San Francisco, CA, USA.

出版信息

Nature. 2025 Apr;640(8059):732-742. doi: 10.1038/s41586-024-08581-9. Epub 2025 Feb 12.

Abstract

The crypt-villus structure of the small intestine serves as an essential protective barrier. The integrity of this barrier is monitored by the complex sensory system of the gut, in which serotonergic enterochromaffin (EC) cells play an important part. These rare sensory epithelial cells surveil the mucosal environment for luminal stimuli and transmit signals both within and outside the gut. However, whether EC cells in crypts and villi detect different stimuli or produce distinct physiological responses is unknown. Here we address these questions by developing a reporter mouse model to quantitatively measure the release and propagation of serotonin from EC cells in live intestines. Crypt EC cells exhibit a tonic low-level mode that activates epithelial serotonin 5-HT receptors to modulate basal ion secretion and a stimulus-induced high-level mode that activates 5-HT receptors on sensory nerve fibres. Both these modes can be initiated by the irritant receptor TRPA1, which is confined to crypt EC cells. The activation of TRPA1 by luminal irritants is enhanced when the protective mucus layer is compromised. Villus EC cells also signal damage through a distinct mechanism, whereby oxidative stress activates TRPM2 channels, which leads to the release of both serotonin and ATP and consequent excitation of sensory nerve fibres. This topological segregation of EC cell functionality along the mucosal architecture constitutes a mechanism for the surveillance, maintenance and protection of gut integrity under diverse physiological conditions.

摘要

小肠的隐窝 - 绒毛结构是一道重要的保护屏障。这一屏障的完整性由肠道复杂的感觉系统监测,其中血清素能肠嗜铬(EC)细胞发挥着重要作用。这些稀少的感觉上皮细胞监测黏膜环境中的腔内刺激,并在肠道内外传递信号。然而,隐窝和绒毛中的EC细胞是否检测不同刺激或产生不同的生理反应尚不清楚。在这里,我们通过开发一种报告基因小鼠模型来定量测量活体肠道中EC细胞血清素的释放和传播,从而解决这些问题。隐窝EC细胞表现出一种持续性低水平模式,该模式激活上皮血清素5 - HT受体以调节基础离子分泌,以及一种刺激诱导的高水平模式,该模式激活感觉神经纤维上的5 - HT受体。这两种模式均可由局限于隐窝EC细胞的刺激性受体TRPA1启动。当保护性黏液层受损时,腔内刺激物对TRPA1的激活会增强。绒毛EC细胞也通过一种独特的机制发出损伤信号,即氧化应激激活TRPM2通道,这会导致血清素和ATP的释放以及随之而来的感觉神经纤维兴奋。EC细胞功能沿黏膜结构的这种拓扑分离构成了在不同生理条件下监测、维持和保护肠道完整性的一种机制。

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