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依赖淋巴管标志物 Prox1 和渗透压的单细胞管延伸途径。

A pathway for unicellular tube extension depending on the lymphatic vessel determinant Prox1 and on osmoregulation.

机构信息

IGBMC, Development and Stem Cells Program, CNRS/INSERM/Université de Strasbourg, Illkirch, France.

出版信息

Nat Cell Biol. 2013 Feb;15(2):157-68. doi: 10.1038/ncb2662. Epub 2013 Jan 20.

Abstract

The mechanisms regulating the extension of small unicellular tubes remain poorly defined. Here we identify several steps in Caenorhabditis elegans excretory canal growth, and propose a model for lumen extension. Our results suggest that the basal and apical excretory membranes grow sequentially: the former extends first like an axon growth cone; the latter extends next as a result of an osmoregulatory activity triggering peri-apical vesicles (a membrane reservoir) to fuse with the lumen. An apical cytoskeletal web including intermediate filaments and actin crosslinking proteins ensures straight regular lumen growth. Expression of several genes encoding proteins mediating excretory lumen extension, such as the osmoregulatory STE20-like kinase GCK-3 and the intermediate filament IFB-1, is regulated by ceh-26 (here referred to as pros-1), which we found essential for excretory canal formation. Interestingly, PROS-1 is homologous to vertebrate Prox1, a transcription factor controlling lymphatic vessel growth. Our findings have potential evolutionary implications for the origin of fluid-collecting organs, and provide a reference for lymphangiogenesis.

摘要

调控小型单细胞管延伸的机制仍未完全明确。在这里,我们鉴定了秀丽隐杆线虫排泄道生长的几个步骤,并提出了管腔延伸的模型。我们的结果表明基底和顶端排泄膜依次生长:前者像轴突生长锥一样延伸;后者由于渗透压调节活动触发周缘囊泡(膜库)与管腔融合而延伸。包括中间丝和肌动蛋白交联蛋白在内的顶端细胞骨架网确保了规则的管腔生长。几种编码参与排泄管腔延伸的蛋白的基因的表达,如渗透压调节 STE20 样激酶 GCK-3 和中间丝 IFB-1,受 ceh-26(这里称为 pros-1)的调控,我们发现 pros-1 对排泄道的形成是必需的。有趣的是,PROS-1 与脊椎动物 Prox1 同源,后者是控制淋巴管生长的转录因子。我们的发现对收集液体的器官的起源具有潜在的进化意义,并为淋巴管生成提供了参考。

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