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Creation of chimeric human/rabbit APOBEC1 with HIV-1 restriction and DNA mutation activities.


ABSTRACT: APOBEC1 (A1) proteins from lagomorphs and rodents have deaminase-dependent restriction activity against HIV-1, whereas human A1 exerts a negligible effect. To investigate these differences in the restriction of HIV-1 by A1 proteins, a series of chimeric proteins combining rabbit and human A1s was constructed. Homology models of the A1s indicated that their activities derive from functional domains that likely act in tandem through a dimeric interface. The C-terminal region containing the leucine-rich motif and the dimerization domains of rabbit A1 is important for its anti-HIV-1 activity. The A1 chimeras with strong anti-HIV-1 activity were incorporated into virions more efficiently than those without anti-HIV-1 activity, and exhibited potent DNA-mutator activity. Therefore, the C-terminal region of rabbit A1 is involved in both its packaging into the HIV-1 virion and its deamination activity against both viral cDNA and genomic RNA. This study identifies the novel molecular mechanism underlying the target specificity of A1.

SUBMITTER: Ikeda T 

PROVIDER: S-EPMC4704027 | biostudies-literature | 2016 Jan

REPOSITORIES: biostudies-literature

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Creation of chimeric human/rabbit APOBEC1 with HIV-1 restriction and DNA mutation activities.

Ikeda Terumasa T   Ong Eugene Boon Beng EB   Watanabe Nobumoto N   Sakaguchi Nobuo N   Maeda Kazuhiko K   Koito Atsushi A  

Scientific reports 20160107


APOBEC1 (A1) proteins from lagomorphs and rodents have deaminase-dependent restriction activity against HIV-1, whereas human A1 exerts a negligible effect. To investigate these differences in the restriction of HIV-1 by A1 proteins, a series of chimeric proteins combining rabbit and human A1s was constructed. Homology models of the A1s indicated that their activities derive from functional domains that likely act in tandem through a dimeric interface. The C-terminal region containing the leucine  ...[more]

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