| Literature DB >> 31740789 |
Viktória Kiss1,2, András Jipa1,2, Kata Varga1, Szabolcs Takáts3,4, Tamás Maruzs1, Péter Lőrincz3,4, Zsófia Simon-Vecsei3, Szilárd Szikora1, István Földi1, Csaba Bajusz1,2, Dávid Tóth1, Péter Vilmos1, Imre Gáspár5, Paolo Ronchi6, József Mihály1, Gábor Juhász7,8.
Abstract
Autophagy ensures the turnover of cytoplasm and requires the coordinated action of Atg proteins, some of which also have moonlighting functions in higher eukaryotes. Here we show that the transmembrane protein Atg9 is required for female fertility, and its loss leads to defects in actin cytoskeleton organization in the ovary and enhances filopodia formation in neurons in Drosophila. Atg9 localizes to the plasma membrane anchor points of actin cables and is also important for the integrity of the cortical actin network. Of note, such phenotypes are not seen in other Atg mutants, suggesting that these are independent of autophagy defects. Mechanistically, we identify the known actin regulators profilin and Ena/VASP as novel binding partners of Atg9 based on microscopy, biochemical, and genetic interactions. Accordingly, the localization of both profilin and Ena depends on Atg9. Taken together, our data identify a new and unexpected role for Atg9 in actin cytoskeleton regulation.Entities:
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Year: 2019 PMID: 31740789 PMCID: PMC7206052 DOI: 10.1038/s41418-019-0452-0
Source DB: PubMed Journal: Cell Death Differ ISSN: 1350-9047 Impact factor: 15.828