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Journal of Zhejiang University-SCIENCE B (Biomedicine & Biotechnology)  2014, Vol. 15 Issue (5): 455-465    DOI: 10.1631/jzus.B1400059
Reviews     
Mechanism and factors that control HIV-1 transcription and latency activation
Rong-diao Liu, Jun Wu, Rui Shao, Yu-hua Xue
School of Pharmaceutical Sciences, Xiamen University, Xiamen 361102, China
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Abstract  After reverse transcription, the HIV-1 proviral DNA is integrated into the host genome and thus subjected to transcription by the host RNA polymerase II (Pol II). With the identification and characterization of human P-TEFb in the late 1990s as a specific host cofactor required for HIV-1 transcription, it is now believed that the elongation stage of Pol II transcription plays a particularly important role in regulating HIV-1 gene expression. HIV-1 uses a sophisticated scheme to recruit human P-TEFb and other cofactors to the viral long terminal repeat (LTR) to produce full-length HIV-1 transcripts. In this process, P-TEFb is regulated by the reversible association with various transcription factors/cofactors to form several multi-subunit complexes (e.g., 7SK snRNP, super elongation complexes (SECs), and the Brd4-P-TEFb complex) that collectively constitute a P-TEFb network for controlling cellular and HIV-1 transcription. Recent progresses in HIV-1 transcription were reviewed in the paper, with the emphasis on the mechanism and factors that control HIV-1 transcription and latency activation.

Key wordsHIV-1      Transcriptional elongation      RNA polymerase II      Tat      P-TEFb     
Received: 28 February 2014      Published: 05 May 2014
CLC:  Q291  
Cite this article:

Rong-diao Liu, Jun Wu, Rui Shao, Yu-hua Xue. Mechanism and factors that control HIV-1 transcription and latency activation. Journal of Zhejiang University-SCIENCE B (Biomedicine & Biotechnology), 2014, 15(5): 455-465.

URL:

http://www.zjujournals.com/xueshu/zjus-b/10.1631/jzus.B1400059     OR     http://www.zjujournals.com/xueshu/zjus-b/Y2014/V15/I5/455

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