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The A-rich RNA sequences of HIV-1 pol are important for the synthesis of viral cDNA

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journal contribution
posted on 2009-01-01, 00:00 authored by C Keating, M Hill, D Hawkes, R Smyth, C Isel, S Y Le, A Palmenberg, J Marshall, R Marquet, G Nabel, Johnson Mak
The bias of A-rich codons in HIV-1 pol is thought to be a record of hypermutations in viral genomes that lack biological functions. Bioinformatic analysis predicted that A-rich sequences are generally associated with minimal local RNA structures. Using codon modifications to reduce the amount of A-rich sequences within HIV-1 genomes, we have reduced the flexibility of RNA sequences in pol to analyze the functional significance of these A-rich ‘structurally poor’ RNA elements in HIV-1 pol. Our data showed that codon modification of HIV-1 sequences led to a suppression of virus infectivity by 5–100-fold, and this defect does not correlate with, viral entry, viral protein expression levels, viral protein profiles or virion packaging of genomic RNA. Codon modification of HIV-1 pol correlated with an enhanced dimer stability of the viral RNA genome, which was associated with a reduction of viral cDNA synthesis both during HIV-1 infection and in a cell free reverse transcription assay. Our data provided direct evidence that the HIV-1 A-rich pol sequence is not merely an evolutionary artifact of enzyme-induced hypermutations, and that HIV-1 has adapted to rely on A-rich RNA sequences to support the synthesis of viral cDNA during reverse transcription, highlighting the utility of using ‘structurally poor’ RNA domains in regulating biological process.

History

Journal

Nucleic acids research

Volume

37

Pagination

945 - 956

Location

Oxford, England

Open access

  • Yes

ISSN

0305-1048

eISSN

1362-4962

Language

eng

Publication classification

C1.1 Refereed article in a scholarly journal

Copyright notice

2009, Oxford University Press