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BMP4/NOGGIN 的差异区室化需要 NOGGIN 的跨上皮转运。

Differential compartmentalization of BMP4/NOGGIN requires NOGGIN trans-epithelial transport.

机构信息

Laboratory of Stem Cell Biology and Molecular Embryology, the Rockefeller University, New York, NY 10065, USA; Center for Studies in Physics and Biology, the Rockefeller University, New York, NY 10065, USA.

Laboratory of Stem Cell Biology and Molecular Embryology, the Rockefeller University, New York, NY 10065, USA.

出版信息

Dev Cell. 2021 Jul 12;56(13):1930-1944.e5. doi: 10.1016/j.devcel.2021.05.003. Epub 2021 May 28.

Abstract

Using self-organizing human models of gastrulation, we previously showed that (1) BMP4 initiates the cascade of events leading to gastrulation, (2) BMP4 signal reception is restricted to the basolateral domain, and (3) in a human-specific manner, BMP4 directly induces the expression of NOGGIN. Here, we report the surprising discovery that in human epiblasts, NOGGIN and BMP4 were secreted into opposite extracellular spaces. Interestingly, apically presented NOGGIN could inhibit basally delivered BMP4. Apically imposed microfluidic flow demonstrated that NOGGIN traveled in the apical extracellular space. Our co-localization analysis detailed the endocytotic route that trafficked NOGGIN from the apical space to the basolateral intercellular space where BMP4 receptors were located. This apical-basal transcytosis was indispensable for NOGGIN inhibition. Taken together, the segregation of activator/inhibitor into distinct extracellular spaces challenges classical views of morphogen movement. We propose that the transport of morphogen inhibitors regulates the spatial availability of morphogens during embryogenesis.

摘要

利用自发组织的人类原肠胚形成模型,我们之前表明:(1)BMP4 启动了导致原肠胚形成的级联事件;(2)BMP4 信号接收仅限于基底外侧域;(3)以人类特有的方式,BMP4 直接诱导 NOGGIN 的表达。在这里,我们报告了一个令人惊讶的发现,即在人类上胚层中,NOGGIN 和 BMP4 被分泌到相反的细胞外空间。有趣的是,顶端呈现的 NOGGIN 可以抑制基底输送的 BMP4。顶端施加的微流控证明,NOGGIN 沿顶端细胞外空间移动。我们的共定位分析详细描述了将 NOGGIN 从顶端空间运输到 BMP4 受体所在的基底细胞间空间的内吞途径。这种顶端-基底的转胞吞对于 NOGGIN 的抑制是必不可少的。总之,激活剂/抑制剂的分隔到不同的细胞外空间挑战了形态发生素运动的经典观点。我们提出,形态发生素抑制剂的运输调节了胚胎发生过程中形态发生素的空间可用性。

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