Core-binding factor subunit beta is not required for non-primate lentiviral Vif-mediated APOBEC3 degradation

Youwei Ai; Dantong Zhu; Cuihui Wang; Chao Su; Jian Ma; Jianzhang Ma; Xiaojun Wang

doi:10.1128/JVI.01924-14

Core-binding factor subunit beta is not required for non-primate lentiviral Vif-mediated APOBEC3 degradation

J Virol. 2014 Oct;88(20):12112-22. doi: 10.1128/JVI.01924-14. Epub 2014 Aug 13.

Authors

Youwei Ai¹, Dantong Zhu¹, Cuihui Wang², Chao Su², Jian Ma², Jianzhang Ma³, Xiaojun Wang⁴

Affiliations

¹ State Key Laboratory of Veterinary Biotechnology, Harbin Veterinary Research Institute, Chinese Academy of Agricultural Sciences, Harbin, China College of Wildlife Resources, Northeast Forestry University, Harbin, China.
² State Key Laboratory of Veterinary Biotechnology, Harbin Veterinary Research Institute, Chinese Academy of Agricultural Sciences, Harbin, China.
³ College of Wildlife Resources, Northeast Forestry University, Harbin, China jianzhangma@163.com xjw@hvri.ac.cn.
⁴ State Key Laboratory of Veterinary Biotechnology, Harbin Veterinary Research Institute, Chinese Academy of Agricultural Sciences, Harbin, China jianzhangma@163.com xjw@hvri.ac.cn.

Abstract

Viral infectivity factor (Vif) is required for lentivirus fitness and pathogenicity, except in equine infectious anemia virus (EIAV). Vif enhances viral infectivity by a Cullin5-Elongin B/C E3 complex to inactivate the host restriction factor APOBEC3. Core-binding factor subunit beta (CBF-β) is a cell factor that was recently shown to be important for the primate lentiviral Vif function. Non-primate lentiviral Vif also degrades APOBEC3 through the proteasome pathway. However, it is unclear whether CBF-β is required for the non-primate lentiviral Vif function. In this study, we demonstrated that the Vifs of non-primate lentiviruses, including feline immunodeficiency virus (FIV), bovine immunodeficiency virus (BIV), caprine arthritis encephalitis virus (CAEV), and maedi-visna virus (MVV), do not interact with CBF-β. In addition, CBF-β did not promote the stability of FIV, BIV, CAEV, and MVV Vifs. Furthermore, CBF-β silencing or overexpression did not affect non-primate lentiviral Vif-mediated APOBEC3 degradation. Our results suggest that non-primate lentiviral Vif induces APOBEC3 degradation through a different mechanism than primate lentiviral Vif. Importance: The APOBEC3 protein family members are host restriction factors that block retrovirus replication. Vif, an accessory protein of lentivirus, degrades APOBEC3 to rescue viral infectivity by forming Cullin5-Elongin B/C-based E3 complex. CBF-β was proved to be a novel regulator of primate lentiviral Vif function. In this study, we found that CBF-β knockdown or overexpression did not affect FIV Vif's function, which induced polyubiquitination and degradation of APOBEC3 by recruiting the E3 complex in a manner similar to that of HIV-1 Vif. We also showed that other non-primate lentiviral Vifs did not require CBF-β to degrade APOBEC3. CBF-β did not interact with non-primate lentiviral Vifs or promote their stability. These results suggest that a different mechanism exists for the Vif-APOBEC interaction and that non-primates are not suitable animal models for exploring pharmacological interventions that disrupt Vif-CBF-β interaction.

Publication types

Research Support, Non-U.S. Gov't

MeSH terms

APOBEC Deaminases
Base Sequence
Core Binding Factor beta Subunit / physiology*
Cytidine Deaminase
Cytosine Deaminase / metabolism*
DNA Primers
Gene Products, vif / physiology*
HEK293 Cells
Humans
Lentivirus / classification
Lentivirus / physiology*
Proteolysis
Reverse Transcriptase Polymerase Chain Reaction

Substances

CBFB protein, human
Core Binding Factor beta Subunit
DNA Primers
Gene Products, vif
Cytosine Deaminase
APOBEC Deaminases
APOBEC3 proteins, human
Cytidine Deaminase