Influence of HIV-1 Genomic RNA on the Formation of Gag Biomolecular Condensates

Influence of HIV-1 Genomic RNA on the Formation of Gag Biomolecular Condensates

[Display omitted] •Gag matrix (MA) domain or the Nucleocapsid (NC) zinc finger motifs alter condensate number and size .•Gag BMCs are bimodally influenced by the HIV-1 viral genomic RNA.•Incubation of Gag with CD4+ T cell nuclear lysates leads to the formation of larger BMCs.•The composition and pro...

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Veröffentlicht in:Journal of molecular biology 2023-08, Vol.435 (16), p.168190-168190, Article 168190
Hauptverfasser: Monette, Anne, Niu, Meijuan, Maldonado, Rebecca Kaddis, Chang, Jordan, Lambert, Gregory S., Flanagan, John M., Cochrane, Alan, Parent, Leslie J., Mouland, Andrew J.
Format: Artikel
Sprache:eng
Schlagworte:
biomolecular condensates
Biomolecular Condensates - metabolism
Biomolecular Condensates - virology
gag Gene Products, Human Immunodeficiency Virus - metabolism
gag polyprotein
Genome, Viral
HIV-1 - genetics
HIV-1 - metabolism
Host-Pathogen Interactions
human immunodeficiency virus-type 1
Humans
phase diagrams
RNA, Viral - genetics
RNA, Viral - metabolism
viral genomic RNA
Virus Assembly
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Zusammenfassung:[Display omitted] •Gag matrix (MA) domain or the Nucleocapsid (NC) zinc finger motifs alter condensate number and size .•Gag BMCs are bimodally influenced by the HIV-1 viral genomic RNA.•Incubation of Gag with CD4+ T cell nuclear lysates leads to the formation of larger BMCs.•The composition and properties of HIV-1 Gag-containing BMCs may be altered by differential association of host factors in nuclear versus cytosolic compartments. Biomolecular condensates (BMCs) play an important role in the replication of a growing number of viruses, but many important mechanistic details remain to be elucidated. Previously, we demonstrated that the pan-retroviral nucleocapsid (NC) and HIV-1 pr55Gag (Gag) proteins phase separate into condensates, and that HIV-1 protease (PR)-mediated maturation of Gag and Gag-Pol precursor proteins yields self-assembling BMCs that have HIV-1 core architecture. Using biochemical and imaging techniques, we aimed to further characterize the phase separation of HIV-1 Gag by determining which of its intrinsically disordered regions (IDRs) influence the formation of BMCs, and how the HIV-1 viral genomic RNA (gRNA) could influence BMC abundance and size. We found that mutations in the Gag matrix (MA) domain or the NC zinc finger motifs altered condensate number and size in a salt-dependent manner. Gag BMCs were also bimodally influenced by the gRNA, with a condensate-promoting regime at lower protein concentrations and a gel dissolution at higher protein concentrations. Interestingly, incubation of Gag with CD4+ T cell nuclear lysates led to the formation of larger BMCs compared to much smaller ones observed in the presence of cytoplasmic lysates. These findings suggest that the composition and properties of Gag-containing BMCs may be altered by differential association of host factors in nuclear and cytosolic compartments during virus assembly. This study significantly advances our understanding of HIV-1 Gag BMC formation and provides a foundation for future therapeutic targeting of virion assembly.
ISSN:0022-2836
1089-8638
1089-8638
DOI:10.1016/j.jmb.2023.168190