| Article ID | Journal | Published Year | Pages | File Type |
|---|---|---|---|---|
| 5533281 | Journal of Molecular Biology | 2017 | 9 Pages |
â¢HIV-1 Vif is a natural APOBEC3G antagonist.â¢Published Vif-derived peptides lack specific APOBEC3G inhibitory activity.â¢Vif peptide 25-39 is simply non-inhibitory.â¢Vif peptide 107-115 inhibits A3G in vitro but is non-specific.
The human APOBEC3G (A3G) enzyme restricts HIV-1 in the absence of the viral accessory protein viral infectivity factor (Vif) by deaminating viral cDNA cytosines to uracils. These uracil lesions base-pair with adenines during the completion of reverse transcription and result in A3G signature G-to-A mutations in the viral genome. Vif protects HIV-1 from A3G-mediated restriction by forming an E3-ubiquitin ligase complex to polyubiquitinate A3G and trigger its degradation. Prior studies indicated that Vif may also directly block the enzymatic activity of A3G and, provocatively, that Vif-derived peptides, Vif 25-39 and Vif 105-119, are similarly inhibitory. Here, we show that Vif 25-39 does not inhibit A3G enzymatic activity and that the inhibitory effect of Vif 105-119 and that of a shorter derivative Vif 107-115, although recapitulated, are non-specific. We also elaborate a simple method for assaying DNA cytosine deaminase activity that eliminates potential polymerase chain reaction-induced biases. Our results show that these Vif-derived peptides are unlikely to be useful as tools to study A3G function or as leads for the development of future therapeutics.
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