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果蝇肌肉中的遗传筛选确定了自噬介导的T小管重塑以及Rab2在自噬中的作用。

Genetic screen in Drosophila muscle identifies autophagy-mediated T-tubule remodeling and a Rab2 role in autophagy.

作者信息

Fujita Naonobu, Huang Wilson, Lin Tzu-Han, Groulx Jean-Francois, Jean Steve, Nguyen Jen, Kuchitsu Yoshihiko, Koyama-Honda Ikuko, Mizushima Noboru, Fukuda Mitsunori, Kiger Amy A

机构信息

Section of Cell and Developmental Biology, Division of Biological Sciences, University of California, San Diego, La Jolla, United States.

Laboratory of Membrane Trafficking Mechanisms, Department of Developmental Biology and Neurosciences, Graduate School of Life Sciences, Tohoku University, Sendai, Japan.

出版信息

Elife. 2017 Jan 7;6:e23367. doi: 10.7554/eLife.23367.

Abstract

Transverse (T)-tubules make-up a specialized network of tubulated muscle cell membranes involved in excitation-contraction coupling for power of contraction. Little is known about how T-tubules maintain highly organized structures and contacts throughout the contractile system despite the ongoing muscle remodeling that occurs with muscle atrophy, damage and aging. We uncovered an essential role for autophagy in T-tubule remodeling with genetic screens of a developmentally regulated remodeling program in Drosophila abdominal muscles. Here, we show that autophagy is both upregulated with and required for progression through T-tubule disassembly stages. Along with known mediators of autophagosome-lysosome fusion, our screens uncovered an unexpected shared role for Rab2 with a broadly conserved function in autophagic clearance. Rab2 localizes to autophagosomes and binds to HOPS complex members, suggesting a direct role in autophagosome tethering/fusion. Together, the high membrane flux with muscle remodeling permits unprecedented analysis both of T-tubule dynamics and fundamental trafficking mechanisms.

摘要

横管(T管)构成了一个由管状肌细胞膜组成的特殊网络,参与兴奋-收缩偶联以产生收缩力。尽管随着肌肉萎缩、损伤和衰老会发生持续的肌肉重塑,但对于T管如何在整个收缩系统中维持高度有序的结构和连接却知之甚少。我们通过对果蝇腹部肌肉中一个受发育调控的重塑程序进行基因筛选,发现了自噬在T管重塑中的重要作用。在这里,我们表明自噬在T管拆卸阶段的进展过程中既被上调,也是其进展所必需的。除了已知的自噬体-溶酶体融合介质外,我们的筛选还发现Rab2在自噬清除中具有广泛保守功能的意外共享作用。Rab2定位于自噬体并与HOPS复合体成员结合,表明其在自噬体拴系/融合中具有直接作用。总之,肌肉重塑过程中的高膜通量使得对T管动力学和基本运输机制进行前所未有的分析成为可能。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/f79a/5249261/efa72ea3d698/elife-23367-fig1.jpg

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