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10.1186/s13578-021-00644-y

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34294141!8295636!34294141
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suck abstract from ncbi


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pmid34294141      Cell+Biosci 2021 ; 11 (1): 140
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  • Genome-wide analysis of protein-protein interactions and involvement of viral proteins in SARS-CoV-2 replication #MMPMID34294141
  • Jiang Y; Tong K; Yao R; Zhou Y; Lin H; Du L; Jin Y; Cao L; Tan J; Zhang XD; Guo D; Pan JA; Peng X
  • Cell Biosci 2021[Jul]; 11 (1): 140 PMID34294141show ga
  • BACKGROUND: Analysis of viral protein-protein interactions is an essential step to uncover the viral protein functions and the molecular mechanism for the assembly of a viral protein complex. We employed a mammalian two-hybrid system to screen all the viral proteins of SARS-CoV-2 for the protein-protein interactions. RESULTS: Our study detected 48 interactions, 14 of which were firstly reported here. Unlike Nsp1 of SARS-CoV, Nsp1 of SARS-CoV-2 has the most interacting partners among all the viral proteins and likely functions as a hub for the viral proteins. Five self-interactions were confirmed, and five interactions, Nsp1/Nsp3.1, Nsp3.1/N, Nsp3.2/Nsp12, Nsp10/Nsp14, and Nsp10/Nsp16, were determined to be positive bidirectionally. Using the replicon reporter system of SARS-CoV-2, we screened all viral Nsps for their impacts on the viral replication and revealed Nsp3.1, the N-terminus of Nsp3, significantly inhibited the replicon reporter gene expression. We found Nsp3 interacted with N through its acidic region at N-terminus, while N interacted with Nsp3 through its NTD, which is rich in the basic amino acids. Furthermore, using purified truncated N and Nsp3 proteins, we determined the direct interactions between Nsp3 and N protein. CONCLUSIONS: Our findings provided a basis for understanding the functions of coronavirus proteins and supported the potential of interactions as the target for antiviral drug development.
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