HIV-1 Vif Protein Blocks the Cytidine Deaminase Activity of B-cell Specific AID in E. Coli by a Similar Mechanism of Action

Overview

Journal Mol Immunol

Specialties Allergy & Immunology
Molecular Biology

Date 2006 Apr 4

PMID 16580072

Citations 13

Authors

Mariana Santa-Marta

Frederico Aires da Silva

Ana Margarida Fonseca

Sylvie Rato

Joao Goncalves

Affiliations

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Abstract

HIV-1 Vif protein protects viral replication in non-permissive cells by inducing degradation of APOBEC3G via ubiquitination and proteasomal pathway, although new studies indicate a putative role in Vif's direct inhibition of APOBEC3G. APOBEC3G is member of a homologous family of proteins with cytidine deaminase activity expressed with characteristic tissue specificity, that in humans consist of APOBEC1, APOBEC2, APOBEC3A-H, APOBEC4 and the activation-induced deaminase (AID), a B lymphoid protein necessary for somatic hypermutation, gene conversion and class switch recombination. In this work we show that Vif can counteract AID's activity in E. coli in absence of specific eukaryotic co-factors necessary for AID induced somatic hypermutation, gene conversion and to stimulate class switch recombination in B-cells. We show that AID inhibition is mediated by a direct protein-protein interaction via unique amino acid D118 an homologous mutant responsible for the species-specific restriction of HIV-1 Vif protein existent for APOBEC3G. These results raise the hypothesis that Vif related proteins can act as a broad inhibitor of deaminase activity. Moreover as AID and Vif evolved in different cellular environments, these results may indicate that Vif related proteins might mimic cellular factors that interact with a structural conserved domain of cytidine deaminases during evolution.

Citing Articles

Impact of HIV-1 Vpr manipulation of the DNA repair enzyme UNG2 on B lymphocyte class switch recombination.

Eldin P, Peron S, Galashevskaya A, Denis-Lagache N, Cogne M, Slupphaug G J Transl Med. 2020; 18(1):310.

PMID: 32778120 PMC: 7418440. DOI: 10.1186/s12967-020-02478-7.

Evasion of adaptive immunity by HIV through the action of host APOBEC3G/F enzymes.

Grant M, Larijani M AIDS Res Ther. 2017; 14(1):44.

PMID: 28893290 PMC: 5594601. DOI: 10.1186/s12981-017-0173-8.

A Novel Regulator of Activation-Induced Cytidine Deaminase/APOBECs in Immunity and Cancer: Schrödinger's CATalytic Pocket.

King J, Larijani M Front Immunol. 2017; 8:351.

PMID: 28439266 PMC: 5382155. DOI: 10.3389/fimmu.2017.00351.

Reassessing APOBEC3G Inhibition by HIV-1 Vif-Derived Peptides.

Richards C, Li M, Perkins A, Rathore A, Harki D, Harris R J Mol Biol. 2016; 429(1):88-96.

PMID: 27887868 PMC: 5186364. DOI: 10.1016/j.jmb.2016.11.012.

Positioning of APOBEC3G/F mutational hotspots in the human immunodeficiency virus genome favors reduced recognition by CD8+ T cells.

Monajemi M, Woodworth C, Zipperlen K, Gallant M, Grant M, Larijani M PLoS One. 2014; 9(4):e93428.

PMID: 24722422 PMC: 3982959. DOI: 10.1371/journal.pone.0093428.