Structural architecture of a dimeric paramyxovirus polymerase complex

Jin Xie,Li Wang, Guanglei Zhai,Daitze Wu, Zhaohu Lin,Manfu Wang,Xiaodong Yan,Lu Gao, Xinyi Huang,Rachel Fearns,Shuai Chen

biorxiv(2021)

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摘要
Human parainfluenza virus type 3 (hPIV3), a member of non-segmented, negative-strand RNA viruses (nsNSVs), is the second most common cause of severe respiratory disease in pediatrics. The transcription and replication processes of nsNSVs are catalyzed by a multi-functional RNA-dependent RNA polymerase (RdRp) complex composed of the large protein (L) and the phosphoprotein (P). Previous studies have shown that the polymerase can adopt a dimeric form, however, the structure of the dimer and how it functions are not understood. Here we determined the cryo-EM structure of hPIV3 L-P complex at 2.7 Å with substantial structural details. A putative catalytic magnesium ion could be built in our structure, and structural comparison revealed atomic features conserved with other RNA viruses. Interactions identified between the two priming and intrusion loops and the connector domain potentially trigger the spatial movement of three C-terminal L domains for different steps of transcription and replication. Structural comparison with other nsNSV RdRps suggests common features of L-P binding. Furthermore, we report for the first time the structural basis of the L-L interaction in the partially modelled dimeric L-P structure, in which the connector domain of one L is positioned at the putative RNA template entry of the other L. Based on these findings, we propose a model by which L dimerization promotes efficient conversion of nascent RNA into a template. ### Competing Interest Statement J.X., L.W., G.Z., D.W., Z.L., L.G., X.H. and S.C. are either current or former employees of Roche Innovation Center Shanghai. The project was funded by Roche Postdoctoral Fellowship in a collaboration with R.F. in Boston University School of Medicine. R.F. also has a sponsored research agreement with Enanta Pharmaceuticals.
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dimeric paramyxovirus polymerase complex
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