Functional divergence of oligoadenylate synthetase 1 (OAS1) proteins in Tetrapods

功能分歧 生物 核糖核酸酶P 遗传学 MDA5型 基因 核糖核酸 RNA干扰 基因组 基因家族
作者
Xiaoxue Wang,Jiaxiang Hu,Linfei Song,Enguang Rong,Chenghuai Yang,Xiaoyun Chen,Juan Pu,Honglei Sun,Chuze Gao,David W. Burt,Jinhua Liu,Ning Li,Yinhua Huang
出处
期刊:Science China-life Sciences [Springer Science+Business Media]
卷期号:65 (7): 1395-1412 被引量:3
标识
DOI:10.1007/s11427-021-2002-y
摘要

OASs play critical roles in immune response against virus infection by polymerizing ATP into 2-5As, which initiate the classical OAS/RNase L pathway and induce degradation of viral RNA. OAS members are functionally diverged in four known innate immune pathways (OAS/RNase L, OASL/IRF7, OASL/RIG-I, and OASL/cGAS), but how they functionally diverged is unclear. Here, we focus on evolutionary patterns and explore the link between evolutionary processes and functional divergence of Tetrapod OAS1. We show that Palaeognathae and Primate OAS1 genes are conserved in genomic and protein structures but differ in function. The former (i.e., ostrich) efficiently synthesized long 2-5A and activated RNase L, while the latter (i.e., human) synthesized short 2-5A and did not activate RNase L. We predicted and verified that two in-frame indels and one positively selected site in the active site pocket contributed to the functional divergence of Palaeognathae and Primate OAS1. Moreover, we discovered and validated that an in-frame indel in the C-terminus of Palaeognathae OAS1 affected the binding affinity of dsRNA and enzymatic activity, and contributed to the functional divergence of Palaeognathae OAS1 proteins. Our findings unravel the molecular mechanism for functional divergence and give insights into the emergence of novel functions in Tetrapod OAS1.
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