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SCRIB 控制上皮分化过程中的顶端收缩性。

SCRIB controls apical contractility during epithelial differentiation.

机构信息

Cell Polarity, Migration and Cancer Unit, Université Paris Cité, UMR3691 CNRS, Institut Pasteur, Paris, France.

Institut de l'Audition, Inserm UMRS 1120, Université Paris Cité, Institut Pasteur, Paris, France.

出版信息

J Cell Biol. 2023 Dec 4;222(12). doi: 10.1083/jcb.202211113. Epub 2023 Nov 6.

Abstract

Although mutations in the SCRIB gene lead to multiple morphological organ defects in vertebrates, the molecular pathway linking SCRIB to organ shape anomalies remains elusive. Here, we study the impact of SCRIB-targeted gene mutations during the formation of the gut epithelium in an organ-on-chip model. We show that SCRIB KO gut-like epithelia are flatter with reduced exposed surface area. Cell differentiation on filters further shows that SCRIB plays a critical role in the control of apical cell shape, as well as in the basoapical polarization of myosin light chain localization and activity. Finally, we show that SCRIB serves as a molecular scaffold for SHROOM2/4 and ROCK1 and identify an evolutionary conserved SHROOM binding site in the SCRIB carboxy-terminal that is required for SCRIB function in the control of apical cell shape. Our results demonstrate that SCRIB plays a key role in epithelial morphogenesis by controlling the epithelial apical contractility during cell differentiation.

摘要

尽管 SCRIB 基因突变会导致脊椎动物多种形态器官缺陷,但 SCRIB 与器官形态异常之间的分子途径仍难以捉摸。在这里,我们在类器官模型中研究了 SCRIB 靶向基因突变在肠道上皮形成过程中的影响。我们发现 SCRIB KO 肠道样上皮更平坦,暴露表面积减少。在过滤器上进行的细胞分化进一步表明,SCRIB 在控制顶端细胞形状以及肌球蛋白轻链定位和活性的基底-顶端极性方面发挥着关键作用。最后,我们表明 SCRIB 充当 SHROOM2/4 和 ROCK1 的分子支架,并鉴定出 SCRIB 羧基末端的一个进化保守的 SHROOM 结合位点,该位点对于 SCRIB 在控制顶端细胞形状中的功能是必需的。我们的研究结果表明,SCRIB 通过在细胞分化过程中控制上皮顶端收缩性在上皮形态发生中发挥关键作用。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/98e2/10626209/e051e8d797f2/JCB_202211113_FigS1.jpg

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