1. Multiple NF-κB Sites in HIV-1 Subtype C Long Terminal Repeat Confer Superior Magnitude of Transcription and Thereby the Enhanced Viral Predominance
- Author
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Nirmala Rajagopalan, Madhu Vajpayee, Venkat S. Yadavalli, Ujjwal Neogi, Anita Shet, Tapas K. Kundu, Udaykumar Ranga, Narayana Cheedarla, Rajesh V. Murali, Raghavendra Bhatt, Shilpee Sharma, Anjali Verma, Anil Babu Mukthey, Swarupa Yalla, Pachamuthu Balakrishnan, Roshan Elizabeth Rajan, Mangaiarkarasi Asokan, Susarla K. Shankar, Kuan-Teh Jeang, Mahesh Bachu, Shanmugam Saravanan, Snehajyoti Chatterjee, Kadappa Shivappa Satish, Anita Mahadevan, and Suniti Solomon
- Subjects
Adult ,Gene Expression Regulation, Viral ,Male ,Transcription, Genetic ,viruses ,Molecular Sequence Data ,HIV Infections ,Biology ,Virus Replication ,Biochemistry ,Cohort Studies ,Young Adult ,Transcription (biology) ,Viral entry ,Gene duplication ,Humans ,Molecular Biology ,HIV Long Terminal Repeat ,Genetics ,NF-kappa B ,Molecular Bases of Disease ,Cell Biology ,Virology ,Long terminal repeat ,Viral replication ,Viral evolution ,HIV-1 ,Female ,Viral load ,Protein Binding - Abstract
We demonstrate that at least three different promoter variant strains of HIV-1 subtype C have been gradually expanding and replacing the standard subtype C viruses in India, and possibly in South Africa and other global regions, over the past decade. The new viral strains contain an additional NF-κB, NF-κB-like, or RBEIII site in the viral promoter. Although the acquisition of an additional RBEIII site is a property shared by all the HIV-1 subtypes, acquiring an additional NF-κB site remains an exclusive property of subtype C. The acquired κB site is genetically distinct, binds the p50-p65 heterodimer, and strengthens the viral promoter at the levels of transcription initiation and elongation. The 4-κB viruses dominate the 3-κB "isogenic" viral strains in pairwise competition assays in T-cell lines, primary cells, and the ecotropic human immunodeficiency virus mouse model. The dominance of the 4-κB viral strains is also evident in the natural context when the subjects are coinfected with κB-variant viral strains. The mean plasma viral loads, but not CD4 counts, are significantly different in 4-κB infection suggesting that these newly emerging strains are probably more infectious. It is possible that higher plasma viral loads underlie selective transmission of the 4-κB viral strains. Several publications previously reported duplication or deletion of diverse transcription factor-binding sites in the viral promoter. Unlike previous reports, our study provides experimental evidence that the new viral strains gained a potential selective advantage as a consequence of the acquired transcription factor-binding sites and importantly that these strains have been expanding at the population level.
- Published
- 2012
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