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SRX12620498: RNA-seq of HIV-1 5'UTR : C84A_C85A_vs_U86G_A89C_Virus_1
1 ILLUMINA (Illumina MiniSeq) run: 55,127 spots, 8.3M bases, 2.7Mb downloads

Design: RT-PCR. single amplicon sequencing using Nextera compatible library preparation strategy
Submitted by: Helmholtz Institute for RNA-based Infection Research
Study: Short and long range interactions in the HIV-1 5 UTR regulate genome dimerization and packaging
show Abstracthide Abstract
Genome dimerization is a conserved feature of retroviral replication and a critical step in the HIV-1 life cycle, but how it is regulated is incompletely understood. Here, we developed FARS-seq (Functional Analysis of RNA Structure) to comprehensively identify sequences and structures within the HIV-1 5 UTR influencing dimerization. We found nucleotides important for dimerization throughout the HIV-1 5 UTR and identified distinct structural conformations in monomeric and dimeric RNA. The dimer displayed TAR, PolyA, PBS, and SL1-SL3 as stem-loops. In the monomer, SL1 was dramatically reconfigured into long- and short-range base-pairings with polyA and PBS, respectively. The polyA-SL1 interaction disrupts the major packaging motifs, and the PBS-SL1 interaction functionally couples the primer binding site with dimerization, Pr55Gag binding and packaging. 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.
Sample:
SAMN22306767 • SRS10575177 • All experiments • All runs
Library:
Name: 210917_C84A_C85A_vs_U86G_A89C_Virus_1
Instrument: Illumina MiniSeq
Strategy: RNA-Seq
Source: VIRAL RNA
Selection: RT-PCR
Layout: PAIRED
Runs: 1 run, 55,127 spots, 8.3M bases, 2.7Mb
Run# of Spots# of BasesSizePublished
SRR1634299355,1278.3M2.7Mb2021-10-14

ID:
17158456

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