Modulation of Autophagy–Lysosome Axis by African Swine Fever Virus and Its Encoded Protein pEP153R

灯1 溶酶体 自噬 非洲猪瘟病毒 细胞生物学 内质网 生物 病毒学 病毒 细胞内 内体 生物化学 细胞凋亡
作者
Siyu Bai,Wenlian Weng,Hua Wang,Zhiying Cui,Jiajun Wu,Yajin Qu,Yuxin Hao,Peng Gao,Yongning Zhang,Lei Zhou,Xinna Ge,Xin Guo,Jun Han,Hanchun Yang
出处
期刊:Current Issues in Molecular Biology [MDPI AG]
卷期号:46 (10): 11236-11254
标识
DOI:10.3390/cimb46100667
摘要

The autophagy–lysosome axis is an evolutionarily conserved intracellular degradation pathway which constitutes an important component of host innate immunity against microbial infections. Here, we show that African swine fever virus (ASFV), one of most devastating pathogens to the worldwide swine industry, can reshape the autophagy–lysosome axis by recruiting the critical lysosome membrane proteins (LAMP1 and LAMP2) to viral factories while inhibiting autophagic induction in macrophages. The screening of viral membrane proteins led to the identification of several ASFV membrane proteins, exemplified by viral protein pEP153R, that could significantly alter the subcellular localization of LAMP1/2 when expressed alone in transfected cells. Further analysis showed that pEP153R was also a component of viral factories and could induce endoplasmic reticulum (ER) retention of LAMP1/2, leading to the inhibition of the fusion of autophagosomes with lysosomes. Interestingly, the ASFV mutant lacking EP153R could still actively recruit LAMP into viral factories (VFs) and inhibit autophagic flux, indicating the existence of a functional redundancy of other viral proteins in the absence of pEP153R and highlighting the complexity of ASFV replication biology. Taken together, our results reveal novel information about the interplay of ASFV with the autophagy–lysosome axis and a previously unrecognized function of ASFV protein pEP153R in regulating the cellular autophagic process.

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