RTKN-1/Rhotekin shields endosome-associated F-actin from disassembly to ensure endocytic recycling |
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Authors: | Yanling Yan Shuai Liu Can Hu Chaoyi Xie Linyue Zhao Shimin Wang Wenjuan Zhang Zihang Cheng Jinghu Gao Xin Fu Zhenrong Yang Xianghong Wang Jing Zhang Long Lin Anbing Shi |
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Affiliation: | 1.Department of Biochemistry and Molecular Biology, School of Basic Medicine, Tongji Medical College, Huazhong University of Science and Technology, Wuhan, Hubei, China;2.Cell Architecture Research Institute, Huazhong University of Science and Technology, Wuhan, Hubei, China |
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Abstract: | ![]() Cargo sorting and the subsequent membrane carrier formation require a properly organized endosomal actin network. To better understand the actin dynamics during endocytic recycling, we performed a genetic screen in C. elegans and identified RTKN-1/Rhotekin as a requisite to sustain endosome-associated actin integrity. Loss of RTKN-1 led to a prominent decrease in actin structures and basolateral recycling defects. Furthermore, we showed that the presence of RTKN-1 thwarts the actin disassembly competence of UNC-60A/cofilin. Consistently, in RTKN-1–deficient cells, UNC-60A knockdown replenished actin structures and alleviated the recycling defects. Notably, an intramolecular interaction within RTKN-1 could mediate the formation of oligomers. Overexpression of an RTKN-1 mutant form that lacks self-binding capacity failed to restore actin structures and recycling flow in rtkn-1 mutants. Finally, we demonstrated that SDPN-1/Syndapin acts to direct the recycling endosomal dwelling of RTKN-1 and promotes actin integrity there. Taken together, these findings consolidated the role of SDPN-1 in organizing the endosomal actin network architecture and introduced RTKN-1 as a novel regulatory protein involved in this process. |
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