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Short- and long-range interactions in the HIV-1 5' UTR regulate genome dimerization and packaging.


ABSTRACT: RNA dimerization is the noncovalent association of two human immunodeficiency virus-1 (HIV-1) genomes. It is a conserved step in the HIV-1 life cycle and assumed to be a prerequisite for binding to the viral structural protein Pr55Gag during genome packaging. Here, we developed functional analysis of RNA structure-sequencing (FARS-seq) to comprehensively identify sequences and structures within the HIV-1 5' untranslated region (UTR) that regulate this critical step. Using FARS-seq, we found nucleotides important for dimerization throughout the HIV-1 5' UTR and identified distinct structural conformations in monomeric and dimeric RNA. In the dimeric RNA, key functional domains, such as stem-loop 1 (SL1), polyadenylation signal (polyA) and primer binding site (PBS), folded into independent structural motifs. In the monomeric RNA, SL1 was reconfigured into long- and short-range base pairings with polyA and PBS, respectively. We show that these interactions disrupt genome packaging, and additionally show that the PBS-SL1 interaction unexpectedly couples the PBS with dimerization and Pr55Gag binding. Altogether, our data provide insights into late stages of HIV-1 life cycle and a mechanistic explanation for the link between RNA dimerization and packaging.

SUBMITTER: Ye L 

PROVIDER: S-EPMC9010304 | biostudies-literature | 2022 Apr

REPOSITORIES: biostudies-literature

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Short- and long-range interactions in the HIV-1 5' UTR regulate genome dimerization and packaging.

Ye Liqing L   Gribling-Burrer Anne-Sophie AS   Bohn Patrick P   Kibe Anuja A   Börtlein Charlene C   Ambi Uddhav B UB   Ahmad Shazeb S   Olguin-Nava Marco M   Smith Maureen M   Caliskan Neva N   von Kleist Max M   Smyth Redmond P RP  

Nature structural & molecular biology 20220328 4


RNA dimerization is the noncovalent association of two human immunodeficiency virus-1 (HIV-1) genomes. It is a conserved step in the HIV-1 life cycle and assumed to be a prerequisite for binding to the viral structural protein Pr55<sup>Gag</sup> during genome packaging. Here, we developed functional analysis of RNA structure-sequencing (FARS-seq) to comprehensively identify sequences and structures within the HIV-1 5' untranslated region (UTR) that regulate this critical step. Using FARS-seq, we  ...[more]

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