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Degradation of the cancer genomic DNA deaminase APOBEC3B by SIV Vif.

Oncotarget. 2015; 
Land AM,, Wang J, Law EK, Aberle R, Kirmaier A, Krupp A,, Johnson WE, Harris RS.
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Codon Optimization … term_id":"210706","term_text":"M32690"}}M32690), MVV 1514 (GenBank {"type":"entrez-nucleotide", "attrs":{"text":"M60610","term_id":"470315","term_text":"M60610"}}M60610), and FIV NSCU (GenBank m25381) were codon optimized (GenScript Corporation) and expressed … Get A Quote

摘要

APOBEC3B is a newly identified source of mutation in many cancers, including breast, head/neck, lung, bladder, cervical, and ovarian. APOBEC3B is a member of the APOBEC3 family of enzymes that deaminate DNA cytosine to produce the pro-mutagenic lesion, uracil. Several APOBEC3 family members function to restrict virus replication. For instance, APOBEC3D, APOBEC3F, APOBEC3G, and APOBEC3H combine to restrict HIV-1 in human lymphocytes. HIV-1 counteracts these APOBEC3s with the viral protein Vif, which targets the relevant APOBEC3s for proteasomal degradation. While APOBEC3B does not restrict HIV-1 and is not targeted by HIV-1 Vif in CD4-positive T cells, we asked whether related lentiviral Vif proteins could degra... More

關鍵詞

APOBEC3B; cancer mutagenesis; endogenous DNA deamination; lentiviral Vif; tumor evolution
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