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Analysis of the N-terminal positively charged residues of the simian immunodeficiency virus Vif reveals a critical amino acid required for the antagonism of rhesus APOBEC3D, G, and H

Virology. 2015; 
Schmitt K, Katuwal M, Wang Y, Li C, Stephens EB.
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Gene Synthesis For expression of the rhesus C (Genbank accession EU381233), D (Genbank accession JF714488), and H (Genbank accession DQ507277) proteins, genes were synthesized by GenScript and subcloned into the pcDNA3.... The rhA3B was based on our analysis of the from the rhesus macaque genome, was synthesized by GenScript and cloned into pcDNA3. Get A Quote

摘要

Previous studies have shown that apolipoprotein B mRNA editing, enzyme catalytic, polypeptide G (APOBEC3G; hA3G) and F (APOBEC3F; hA3F) proteins interact with a nonlinear binding site located at the N-terminal region of the HIV-1 Vif protein. We have analyzed the role of 12 positively charged amino acids of the N-terminal region of the SIV Vif. Simian-human immunodeficiency viruses (SHIV) were constructed that expressed each of these amino acid substitutions. These viruses were examined for replication in the presence of rhesus macaque APOBEC3 proteins (rhA3A-rhA3H), incorporation of the different A3 proteins into virions, and replication in rhesus macaque PBMC. Similar to other studies, we found that K27 was e... More

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