Abstract

The 5'-untranslated leader region of human immunodeficiency virus type 1 (HIV-1) RNA contains multiple signals that control distinct steps of the viral replication cycle such as transcription, reverse transcription, genomic RNA dimerization, splicing, and packaging. It is likely that fine tuned coordinated regulation of these functions is achieved through specific RNA-protein and RNA-RNA interactions. In a search for cis-acting elements important for the tertiary structure of the 5'-untranslated region of HIV-1 genomic RNA, we identified, by ladder selection experiments, a short stretch of nucleotides directly downstream of the poly(A) signal that interacts with a nucleotide sequence located in the matrix region. Confirmation of the sequence of the interacting sites was obtained by partial or complete inhibition of this interaction by antisense oligonucleotides and by nucleotide substitutions. In the wild type RNA, this long range interaction was intramolecular, since no intermolecular RNA association was detected by gel electrophoresis with an RNA mutated in the dimerization initiation site and containing both sequences involved in the tertiary interaction. Moreover, the functional importance of this interaction is supported by its conservation in all HIV-1 isolates as well as in HIV-2 and simian immunodeficiency virus. Our results raise the possibility that this long range RNA-RNA interaction might be involved in the full-length genomic RNA selection during packaging, repression of the 5' polyadenylation signal, and/or splicing regulation.

Highlights

  • The genomes of RNA viruses are multifunctional molecules

  • In a search for cis-acting elements important for the tertiary structure of the 5؅untranslated region of human immunodeficiency virus type 1 (HIV-1) genomic RNA, we identified, by ladder selection experiments, a short stretch of nucleotides directly downstream of the poly(A) signal that interacts with a nucleotide sequence located in the matrix region

  • RNA Sequences Upstream and Downstream of the SD Site Interact Together—It has previously been reported by us (25, 26, 39) and by others (22, 23) that the 5Ј-untranslated region of HIV-1 genomic RNA contains the major dimerization signal (DIS) but that other regions around the DIS could influence the scaffold of the RNA tertiary structure (24, 40)

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Summary

Introduction

The genomes of RNA viruses are multifunctional molecules. In retroviruses, including human immunodeficiency virus type 1 (HIV-1),1 the primary RNA transcript functions as pre-mRNA (splicing), mRNA (synthesis of Gag and Gag-Pol proteins), and genomic RNA for packaging into infectious particles. In a search for cis-acting elements important for the tertiary structure of the 5Ј-unstranslated region of HIV-1 genomic RNA, we used ladder selection experiments to identify a short stretch of nucleotides directly downstream of the poly(A) signal that interacts with a nucleotide sequence located in the matrix coding region.

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