Assembly of the Tripartite and RNA Condensates of the Respiratory Syncytial Virus Factory Proteins IIn Vitro/I: Role of the Transcription Antiterminator M[sub.2-1]

A wide variety of viruses replicate in liquid-like viral factories. Non-segmented negative stranded RNA viruses share a nucleoprotein (N) and a phosphoprotein (P) that together emerge as the main drivers of liquid–liquid phase separation. The respiratory syncytial virus includes the transcription an...

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Veröffentlicht in:Viruses 2023-06, Vol.15 (6)
Hauptverfasser: Visentin, Araceli, Demitroff, Nicolás, Salgueiro, Mariano, Borkosky, Silvia Susana, Uversky, Vladimir N, Camporeale, Gabriela, de Prat-Gay, Gonzalo
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Sprache:eng
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Zusammenfassung:A wide variety of viruses replicate in liquid-like viral factories. Non-segmented negative stranded RNA viruses share a nucleoprotein (N) and a phosphoprotein (P) that together emerge as the main drivers of liquid–liquid phase separation. The respiratory syncytial virus includes the transcription antiterminator M[sub.2-1] , which binds RNA and maximizes RNA transcriptase processivity. We recapitulate the assembly mechanism of condensates of the three proteins and the role played by RNA. M[sub.2-1] displays a strong propensity for condensation by itself and with RNA through the formation of electrostatically driven protein–RNA coacervates based on the amphiphilic behavior of M[sub.2-1] and finely tuned by stoichiometry. M[sub.2-1] incorporates into tripartite condensates with N and P, modulating their size through an interplay with P, where M[sub.2-1] is both client and modulator. RNA is incorporated into the tripartite condensates adopting a heterogeneous distribution, reminiscent of the M[sub.2-1] -RNA IBAG granules within the viral factories. Ionic strength dependence indicates that M[sub.2-1] behaves differently in the protein phase as opposed to the protein–RNA phase, in line with the subcompartmentalization observed in viral factories. This work dissects the biochemical grounds for the formation and fate of the RSV condensates in vitro and provides clues to interrogate the mechanism under the highly complex infection context.
ISSN:1999-4915
1999-4915
DOI:10.3390/v15061329