Literature DB >> 27834211

Transcriptional start site heterogeneity modulates the structure and function of the HIV-1 genome.

Siarhei Kharytonchyk1, Sarah Monti2, Philip J Smaldino1, Verna Van2, Nicholas C Bolden2, Joshua D Brown2, Emily Russo2, Canessa Swanson2, Alex Shuey2, Alice Telesnitsky3, Michael F Summers4,5.   

Abstract

The promoter in HIV type 1 (HIV-1) proviral DNA contains three sequential guanosines at the U3-R boundary that have been proposed to function as sites for transcription initiation. Here we show that all three sites are used in cells infected with HIV-1 and that viral RNAs containing a single 5' capped guanosine (Cap1G) are specifically selected for packaging in virions, consistent with a recent report [Masuda et al. (2015) Sci Rep 5:17680]. In addition, we now show that transcripts that begin with two or three capped guanosines (Cap2G or Cap3G) are enriched on polysomes, indicating that RNAs synthesized from different transcription start sites have different functions in viral replication. Because genomes are selected for packaging as dimers, we examined the in vitro monomer-dimer equilibrium properties of Cap1G, Cap2G, and Cap3G 5'-leader RNAs in the NL4-3 strain of HIV-1. Strikingly, under physiological-like ionic conditions in which the Cap1G 5'-leader RNA adopts a dimeric structure, the Cap2G and Cap3G 5'-leader RNAs exist predominantly as monomers. Mutagenesis studies designed to probe for base-pairing interactions suggest that the additional guanosines of the 2G and 3G RNAs remodel the base of the PolyA hairpin, resulting in enhanced sequestration of dimer-promoting residues and stabilization of the monomer. Our studies suggest a mechanism through which the structure, function, and fate of the viral genome can be modulated by the transcriptionally controlled presence or absence of a single 5' guanosine.

Entities:  

Keywords:  5′-leader; HIV-1; RNA; structure; transcription

Mesh:

Substances:

Year:  2016        PMID: 27834211      PMCID: PMC5127319          DOI: 10.1073/pnas.1616627113

Source DB:  PubMed          Journal:  Proc Natl Acad Sci U S A        ISSN: 0027-8424            Impact factor:   11.205


  52 in total

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Journal:  Proc Natl Acad Sci U S A       Date:  2016-10-10       Impact factor: 11.205

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  46 in total

1.  Structural basis for transcriptional start site control of HIV-1 RNA fate.

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Authors:  Brook C Barajas; Motoko Tanaka; Bridget A Robinson; Daryl J Phuong; Kasana Chutiraka; Jonathan C Reed; Jaisri R Lingappa
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4.  Flexibility in Nucleic Acid Binding Is Central to APOBEC3H Antiviral Activity.

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5.  Visualizing the translation and packaging of HIV-1 full-length RNA.

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6.  Epitranscriptomic Addition of m5C to HIV-1 Transcripts Regulates Viral Gene Expression.

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7.  Influence of gag and RRE Sequences on HIV-1 RNA Packaging Signal Structure and Function.

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8.  N6-Methyladenosine-binding proteins suppress HIV-1 infectivity and viral production.

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Review 9.  Alternate RNA Structures.

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10.  Moloney Murine Leukemia Virus p12 Is Required for Histone Loading onto Retroviral DNAs.

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