He Xing, Jin Shouheng
Guangdong Province Key Laboratory of Pharmaceutical Functional Genes, MOE Key Laboratory of Gene Function and Regulation, State Key Laboratory of Biocontrol, School of Life Sciences, Sun Yat-sen University, Guangzhou, Guangdong, China.
Autophagy. 2025 Feb;21(2):492-493. doi: 10.1080/15548627.2024.2431341. Epub 2024 Nov 27.
Reticulophagy selectively degrades fragments of the endoplasmic reticulum (ER) through macroautophagy/autophagy to maintain ER homeostasis. The deficiency of reticulophagy results in the unfolded protein response (UPR), which is a crucial clue to the pathogenesis of inflammatory diseases. However, the detailed mechanism underlying the cross-regulation between reticulophagy and inflammatory diseases remains largely unclear. Recently, we have revealed that UBAC2 (UBA domain containing 2) is essential for controlling ER homeostasis as a novel reticulophagy receptor. MARK2 catalyzes the phosphorylation of UBAC2 at serine (S) 223, hence facilitating the progression of reticulophagy and inhibiting ER stress-induced inflammatory responses.
网状自噬通过巨自噬/自噬选择性降解内质网(ER)片段以维持内质网稳态。网状自噬缺陷会导致未折叠蛋白反应(UPR),这是炎症性疾病发病机制的关键线索。然而,网状自噬与炎症性疾病之间交叉调节的详细机制仍不清楚。最近,我们发现UBAC2(含UBA结构域2)作为一种新型网状自噬受体,对于控制内质网稳态至关重要。MARK2催化UBAC2丝氨酸(S)223位点的磷酸化,从而促进网状自噬进程并抑制内质网应激诱导的炎症反应。
