RTN3L and CALCOCO1 function in parallel to maintain proteostasis in the endoplasmic reticulum.

Autophagy Pub Date : 2024-09-01 Epub Date: 2024-05-31 DOI:10.1080/15548627.2024.2353502
Kamal Kumar, Ravi Chidambaram, Smriti Parashar, Susan Ferro-Novick
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Abstract

Reticulophagy is mediated by autophagy receptors that function in one of the two domains of the ER, tubules or flat sheets. Three different conserved mammalian receptors mediate autophagy in ER tubules: RTN3L, ATL3 and CALCOCO1. Previous studies have shown that RTN3L maintains proteostasis by targeting mutant aggregation-prone proteins for autophagy at distinct foci in ER tubules that we named ERPHS (ER-reticulophagy sites). The role for ATL3 and CALCOCO1 in proteostasis has not been addressed. Here we analyzed three different misfolded disease-causing RTN3L substrates and show that ATL3 and CALCOCO1 target the same cargoes for autophagy. Colocalization and knock down studies revealed that RTN3L and ATL3 are both required for the formation of RTN3L-containing ERPHS, while CALCOCO1 is not. We propose that RTN3L, ATL3 and CALCOCO1 work in parallel to maintain proteostasis within the ER network by targeting cargoes at different sites in the tubules.Abbreviation ATL3: atlastin GTPase 3; Baf: bafilomycin A1; CALCOCO1: calcium binding and coiled-coil domain 1; Epr1: ER-phagy receptor 1; ER: endoplasmic reticulum; ERAD: ER-associated protein degradation; ERPHS: ER-reticulophagy sites; LAMP1: lysosomal associated membrane protein 1; PGRMC1: progesterone receptor membrane component 1; POMC: proopiomelanocortin; Pro-AVP: pro-arginine vasopressin; RETREG1: reticulophagy regulator 1; reticulophagy: endoplasmic reticulum selective autophagy; RTN3L: reticulon 3 long isoform; VAPA: VAMP associated protein A.

RTN3L 和 CALCOCO1 同时发挥作用,维持内质网中的蛋白稳态。
网状吞噬是由自噬受体介导的,这些受体在ER的两个结构域(管状结构域或扁平结构域)之一发挥作用。三种不同的哺乳动物保守受体介导 ER 小管中的自噬:RTN3L、ATL3 和 CALCOCO1。先前的研究表明,RTN3L 通过将突变的易聚集蛋白靶向ER小管中的不同病灶进行自噬来维持蛋白稳态,我们将这些病灶命名为ERPHS(ER-reticulophagy sites)。ATL3 和 CALCOCO1 在蛋白稳态中的作用尚未得到研究。在这里,我们分析了三种不同的错误折叠致病 RTN3L 底物,结果表明 ATL3 和 CALCOCO1 以相同的货物为自噬目标。共定位和基因敲除研究显示,RTN3L 和 ATL3 都是形成含 RTN3L 的 ERPHS 所必需的,而 CALCOCO1 则不是。我们建议 RTN3L、ATL3 和 CALCOCO1 并行工作,通过在小管的不同位点靶向货物来维持 ER 网络内的蛋白稳态。缩写 ATL3:atlastin GTPase 3;Baf:bafilomycin A1;CALCOCO1:钙结合和线圈结构域 1;Epr1:ER-吞噬受体 1:ERAD:ER 相关蛋白降解;ERPHS:ER-reticulophagy sites;LAMP1:溶酶体相关膜蛋白 1;PGRMC1:孕酮受体膜成分 1;POMC:RETREG1:网状吞噬调节因子 1;网状吞噬:内质网选择性自噬;RTN3L:网状细胞 3 长异构体;VAPA:VAMP:VAMP 相关蛋白 A。
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