Scaffold attachment factor B suppresses HIV-1 infection of CD4+ T cells by preventing binding of RNA polymerase II to HIV-1's long terminal repeat

Li Ma; Li Sun; Xia Jin; Si-Dong Xiong; Jian-Hua Wang

doi:10.1074/jbc.RA118.002018

Scaffold attachment factor B suppresses HIV-1 infection of CD4⁺ T cells by preventing binding of RNA polymerase II to HIV-1's long terminal repeat

J Biol Chem. 2018 Aug 3;293(31):12177-12185. doi: 10.1074/jbc.RA118.002018. Epub 2018 Jun 10.

Authors

Li Ma¹, Li Sun², Xia Jin², Si-Dong Xiong³, Jian-Hua Wang⁴

Affiliations

¹ Jiangsu Key Laboratory of Infection and Immunity, Institutes of Biology and Medical Sciences, Soochow University, Suzhou 215006, China; Chinese Academy of Sciences Key Laboratory of Molecular Virology and Immunology, Institute Pasteur of Shanghai, Chinese Academy of Sciences, Shanghai 200031, China.
² Chinese Academy of Sciences Key Laboratory of Molecular Virology and Immunology, Institute Pasteur of Shanghai, Chinese Academy of Sciences, Shanghai 200031, China.
³ Jiangsu Key Laboratory of Infection and Immunity, Institutes of Biology and Medical Sciences, Soochow University, Suzhou 215006, China.
⁴ Chinese Academy of Sciences Key Laboratory of Molecular Virology and Immunology, Institute Pasteur of Shanghai, Chinese Academy of Sciences, Shanghai 200031, China. Electronic address: jh_wang@sibs.ac.cn.

Abstract

The 5' end of the HIV, type 1 (HIV-1) long terminal repeat (LTR) promoter plays an essential role in driving viral transcription and productive infection. Multiple host and viral factors regulate LTR activity and modulate HIV-1 latency. Manipulation of the HIV-1 LTR provides a potential therapeutic strategy for combating HIV-1 persistence. In this study, we identified an RNA/DNA-binding protein, scaffold attachment factor B (SAFB1), as a host cell factor that represses HIV-1 transcription. We found that SAFB1 bound to the HIV-1 5' LTR and significantly repressed 5' LTR-driven viral transcription and HIV-1 infection of CD4⁺ T cells. Mechanistically, SAFB1-mediated repression of HIV-1 transcription and infection was independent of its RNA- and DNA-binding capacities. Instead, by binding to phosphorylated RNA polymerase II, SAFB1 blocked its recruitment to the HIV-1 LTR. Of note, SAFB1-mediated repression of HIV-1 transcription from proviral DNA maintained HIV-1 latency in CD4⁺ T cells. In summary, our findings reveal that SAFB1 binds to the HIV-1 LTR and physically interacts with phosphorylated RNA polymerase II, repressing HIV-1 transcription initiation and elongation. Our findings improve our understanding of host modulation of HIV-1 transcription and latency and provide a new host cell target for improved anti-HIV-1 therapies.

Keywords: HIV; host–pathogen interaction; viral transcription; virology; virus.

Publication types

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

MeSH terms

CD4-Positive T-Lymphocytes / enzymology
CD4-Positive T-Lymphocytes / metabolism
CD4-Positive T-Lymphocytes / virology*
Down-Regulation
Gene Expression Regulation, Viral
HIV Infections / enzymology
HIV Infections / genetics
HIV Infections / metabolism*
HIV Infections / virology
HIV Long Terminal Repeat*
HIV-1 / genetics
HIV-1 / physiology*
Host-Pathogen Interactions
Humans
Matrix Attachment Region Binding Proteins / genetics
Matrix Attachment Region Binding Proteins / metabolism*
Nuclear Matrix-Associated Proteins / genetics
Nuclear Matrix-Associated Proteins / metabolism*
Protein Binding
Proviruses / genetics
Proviruses / physiology
RNA Polymerase II / genetics
RNA Polymerase II / metabolism*
Receptors, Estrogen / genetics
Receptors, Estrogen / metabolism*
Transcription, Genetic
Virus Latency

Substances

Matrix Attachment Region Binding Proteins
Nuclear Matrix-Associated Proteins
Receptors, Estrogen
SAFB protein, human
RNA Polymerase II