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WHAMM在肾脏重吸收中发挥作用,并使肌动蛋白聚合以促进自噬体膜的封闭和货物隔离。

WHAMM functions in kidney reabsorption and polymerizes actin to promote autophagosomal membrane closure and cargo sequestration.

作者信息

Coulter Alyssa M, Cortés Valerie, Theodore Corey J, Cianciolo Rachel E, Korstanje Ron, Campellone Kenneth G

机构信息

Department of Molecular & Cell Biology, Institute for Systems Genomics; University of Connecticut, Storrs CT, USA.

The Jackson Laboratory, Bar Harbor ME, USA.

出版信息

bioRxiv. 2024 Jan 23:2024.01.22.576497. doi: 10.1101/2024.01.22.576497.

Abstract

The actin cytoskeleton is essential for many functions of eukaryotic cells, but the factors that nucleate actin assembly are not well understood at the organismal level or in the context of disease. To explore the function of the actin nucleation factor WHAMM in mice, we examined how inactivation impacts kidney physiology and cellular proteostasis. We show that male WHAMM knockout mice excrete elevated levels of albumin, glucose, phosphate, and amino acids, and display abnormalities of the kidney proximal tubule, suggesting that WHAMM activity is important for nutrient reabsorption. In kidney tissue, the loss of WHAMM results in the accumulation of the lipidated autophagosomal membrane protein LC3, indicating an alteration in autophagy. In mouse fibroblasts and human proximal tubule cells, WHAMM and its binding partner the Arp2/3 complex control autophagic membrane closure and cargo receptor recruitment. These results reveal a role for WHAMM-mediated actin assembly in maintaining kidney function and promoting proper autophagosome membrane remodeling.

摘要

肌动蛋白细胞骨架对真核细胞的多种功能至关重要,但在生物体水平或疾病背景下,引发肌动蛋白组装的因素尚不清楚。为了探究肌动蛋白成核因子WHAMM在小鼠中的功能,我们研究了其失活如何影响肾脏生理和细胞蛋白质稳态。我们发现雄性WHAMM基因敲除小鼠排泄的白蛋白、葡萄糖、磷酸盐和氨基酸水平升高,并表现出肾近端小管异常,这表明WHAMM活性对营养物质重吸收很重要。在肾脏组织中,WHAMM的缺失导致脂化自噬体膜蛋白LC3积累,表明自噬发生改变。在小鼠成纤维细胞和人近端小管细胞中,WHAMM及其结合伴侣Arp2/3复合物控制自噬膜封闭和货物受体募集。这些结果揭示了WHAMM介导的肌动蛋白组装在维持肾脏功能和促进自噬体膜正常重塑中的作用。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/69dc/10849548/b0285117559b/nihpp-2024.01.22.576497v1-f0001.jpg

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