ER-phagy 通过其受体 UBAC2 抑制炎症反应。

Xing He,Haowei He,Zitong Hou,Zheyu Wang,Qinglin Shi,Tao Zhou,Yaoxing Wu,Yunfei Qin,Jun Wang,Zhe Cai,Jun Cui,Shouheng Jin
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引用次数: 0

摘要

ER吞噬是内质网(ER)碎片的一种选择性自噬降解形式,在调节ER平衡方面发挥着至关重要的作用。ER吞噬失调与未折叠蛋白反应(UPR)有关,而UPR是诱发炎症性疾病的主要线索。然而,ER-噬菌体与疾病之间联系的分子机制仍未明确。在这里,我们发现了含有泛素相关结构域的蛋白2(UBAC2),它是ER吞噬的受体,同时也是炎症反应的负调控因子。UBAC2的细胞质结构域中含有一个典型的LC3相互作用区(LIR),可与自噬体GABARAP结合。当ER应激或自噬激活时,微管亲和性调节激酶2(MARK2)会使UBAC2的丝氨酸(S)223磷酸化,促进其二聚化。二聚化的 UBAC2 与 GABARAP 的相互作用更强,从而促进了 ER 的选择性降解。此外,通过影响ER吞噬,UBAC2抑制了小鼠的炎症反应和急性溃疡性结肠炎(UC)。我们的研究结果表明,MARK2-UBAC2轴引导的ER吞噬可能为炎症性疾病的治疗提供靶点。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
ER-phagy restrains inflammatory responses through its receptor UBAC2.
ER-phagy, a selective form of autophagic degradation of endoplasmic reticulum (ER) fragments, plays an essential role in governing ER homeostasis. Dysregulation of ER-phagy is associated with the unfolded protein response (UPR), which is a major clue for evoking inflammatory diseases. However, the molecular mechanism underpinning the connection between ER-phagy and disease remains poorly defined. Here, we identified ubiquitin-associated domain-containing protein 2 (UBAC2) as a receptor for ER-phagy, while at the same time being a negative regulator of inflammatory responses. UBAC2 harbors a canonical LC3-interacting region (LIR) in its cytoplasmic domain, which binds to autophagosomal GABARAP. Upon ER-stress or autophagy activation, microtubule affinity-regulating kinase 2 (MARK2) phosphorylates UBAC2 at serine (S) 223, promoting its dimerization. Dimerized UBAC2 interacts more strongly with GABARAP, thus facilitating selective degradation of the ER. Moreover, by affecting ER-phagy, UBAC2 restrains inflammatory responses and acute ulcerative colitis (UC) in mice. Our findings indicate that ER-phagy directed by a MARK2-UBAC2 axis may provide targets for the treatment of inflammatory disease.
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