Molecular and functional interactions of cat APOBEC3 and feline foamy and immunodeficiency virus proteins: different ways to counteract host-encoded restriction |
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Authors: | Chareza Sarah Slavkovic Lukic Dragana Liu Yang Räthe Ann-Mareen Münk Carsten Zabogli Elisa Pistello Mauro Löchelt Martin |
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Affiliation: | a German Cancer Research Center (DKFZ), Research Program Infection and Cancer, Heidelberg, Germanyb Clinic for Gasteroenterology, Hepatology and Infectiology, Medical Faculty, Heinrich-Heine-University, Düsseldorf, Germanyc Retrovirus Center, University of Pisa, Italy |
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Abstract: | Defined host-encoded feline APOBEC3 (feA3) cytidine deaminases efficiently restrict the replication and spread of exogenous retroviruses like Feline Immunodeficiency Virus (FIV) and Feline Foamy Virus (FFV) which developed different feA3 counter-acting strategies. Here we characterize the molecular interaction of FFV proteins with the diverse feA3 proteins. The FFV accessory protein Bet is the virus-encoded defense factor which is shown here to bind all feA3 proteins independent of whether they restrict FFV, a feature shared with FIV Vif that induces degradation of all feA3s including those that do not inactivate FIV. In contrast, only some feA3 proteins bind to FFV Gag, a pattern that in part reflects the restriction pattern detected. Additionally, one-domain feA3 proteins can homo- and hetero-dimerize in vitro, but a trans-dominant phenotype of any of the low-activity feA3 forms on FFV restriction by one of the highly-active feA3Z2 proteins was not detectable. |
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Keywords: | Foamy virus Feline immunodeficiency virus Anti-viral restriction APOBEC3 cytidine deaminase Bet protein Vif protein |
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