Recruitment of autophagy initiator TAX1BP1 advances aggrephagy from cargo collection to sequestration.

Bernd Bauer,Jonas Idinger,Martina Schuschnig,Luca Ferrari,Sascha Martens
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Abstract

Autophagy mediates the degradation of harmful material within lysosomes. In aggrephagy, the pathway mediating the degradation of aggregated, ubiquitinated proteins, this cargo material is collected in larger condensates prior to its sequestration by autophagosomes. In this process, the autophagic cargo receptors SQSTM1/p62 and NBR1 drive cargo condensation, while TAX1BP1, which binds to NBR1, recruits the autophagy machinery to facilitate autophagosome biogenesis at the condensates. The mechanistic basis for the TAX1BP1-mediated switch from cargo collection to its sequestration is unclear. Here we show that TAX1BP1 is not a constitutive component of the condensates. Its recruitment correlates with the induction of autophagosome biogenesis. TAX1BP1 is sufficient to recruit the TBK1 kinase via the SINTBAD adapter. We define the NBR1-TAX1BP1-binding site, which is adjacent to the GABARAP/LC3 interaction site, and demonstrate that the recruitment of TAX1BP1 to cargo mimetics can be enhanced by an increased ubiquitin load. Our study suggests that autophagosome biogenesis is initiated once sufficient cargo is collected in the condensates.
自噬启动子 TAX1BP1 的招募将凝集作用从货物收集推进到螯合。
自噬介导溶酶体内有害物质的降解。在介导降解聚集的泛素化蛋白质的途径--aggrephagy 中,这种货物物质在被自噬体封存之前会聚集成较大的凝结物。在这一过程中,自噬货物受体 SQSTM1/p62 和 NBR1 驱动货物凝聚,而与 NBR1 结合的 TAX1BP1 则招募自噬机制,促进凝聚体处的自噬体生物生成。目前还不清楚 TAX1BP1 介导的从货物收集到货物封存转换的机理基础。在这里,我们发现 TAX1BP1 并非凝聚体的组成成分。它的招募与自噬体生物生成的诱导相关。TAX1BP1 足以通过 SINTBAD 适配器招募 TBK1 激酶。我们定义了NBR1-TAX1BP1结合位点,该位点毗邻GABARAP/LC3相互作用位点,并证明TAX1BP1对货物模拟物的招募可通过增加泛素负荷而增强。我们的研究表明,一旦冷凝物中收集到足够的货物,自噬体的生物生成就开始了。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
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