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作 者:Baisong Zheng Xiaolei Zhou Li Tian Jian Wang Wenyan Zhang
出 处:《Virologica Sinica》2022年第5期676-684,共9页中国病毒学(英文版)
基 金:supported by funding from the National Key R&D Program of China (2021YFC2301900 and 2301904);National Natural Science Foundation of China (81930062);Science and Technology Department of Jilin Province (YDZJ202201ZYTS590);Health Commission of Jilin Province (2020J059);the Key Laboratory of Molecular Virology,Jilin Province (20102209)
摘 要:Enterovirus 71(EV71) caused hand, foot and mouth disease(HFMD) is a serious threat to the health of young children. Although type I interferon(IFN-I) has been proven to control EV71 replication, the key downstream IFNstimulated gene(ISG) remains to be clarified and investigated. Recently, we found that 2’-5’-oligoadenylate synthetases 3(OAS3), as one of ISG of IFN-β1b, was antagonized by EV71 3C protein. Here, we confirm that OAS3is the major determinant of IFN-β1b-mediated EV71 inhibition, which depends on the downstream constitutive RNase L activation. 2’-5’-oligoadenylate(2-5A) synthesis activity deficient mutations of OAS3 D816A, D818A,D888A, and K950A lost resistance to EV71 because they could not activate downstream RNase L. Further investigation proved that EV71 infection induced OAS3 but not RNase L expression by IFN pathway. Mechanically, EV71 or IFN-β1b-induced phosphorylation of STAT1, but not STAT3, initiated the transcription of OAS3 by directly binding to the OAS3 promoter. Our works elucidate the immune regulatory mechanism of the host OAS3/RNase L system against EV71 replication.
关 键 词:Enterovirus 71(EV71) 20-50-oligoadenylate synthetases 3(OAS3) RNase L IFN-β1b JAK/STAT
分 类 号:R373.2[医药卫生—病原生物学]
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