New Perspectives on the Biogenesis of Viral Inclusion Bodies in Negative-Sense RNA Virus Infections

Infections by negative strand RNA viruses (NSVs) induce the formation of viral inclusion bodies (IBs) in the host cell that segregate viral as well as cellular proteins to enable efficient viral replication. The induction of those membrane-less viral compartments leads inevitably to structural remod...

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Main Authors: Olga Dolnik, Gesche K. Gerresheim, Nadine Biedenkopf
Format: Article
Language:English
Published: MDPI AG 2021-06-01
Series:Cells
Subjects:
Online Access:https://www.mdpi.com/2073-4409/10/6/1460
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spelling doaj-21b71f6001dd4bee857d27af66846f4b2021-06-30T23:51:09ZengMDPI AGCells2073-44092021-06-01101460146010.3390/cells10061460New Perspectives on the Biogenesis of Viral Inclusion Bodies in Negative-Sense RNA Virus InfectionsOlga Dolnik0Gesche K. Gerresheim1Nadine Biedenkopf2Institute for Virology, Philipps-University Marburg, 35043 Marburg, GermanyInstitute for Virology, Philipps-University Marburg, 35043 Marburg, GermanyInstitute for Virology, Philipps-University Marburg, 35043 Marburg, GermanyInfections by negative strand RNA viruses (NSVs) induce the formation of viral inclusion bodies (IBs) in the host cell that segregate viral as well as cellular proteins to enable efficient viral replication. The induction of those membrane-less viral compartments leads inevitably to structural remodeling of the cellular architecture. Recent studies suggested that viral IBs have properties of biomolecular condensates (or liquid organelles), as have previously been shown for other membrane-less cellular compartments like stress granules or P-bodies. Biomolecular condensates are highly dynamic structures formed by liquid-liquid phase separation (LLPS). Key drivers for LLPS in cells are multivalent protein:protein and protein:RNA interactions leading to specialized areas in the cell that recruit molecules with similar properties, while other non-similar molecules are excluded. These typical features of cellular biomolecular condensates are also a common characteristic in the biogenesis of viral inclusion bodies. Viral IBs are predominantly induced by the expression of the viral nucleoprotein (N, NP) and phosphoprotein (P); both are characterized by a special protein architecture containing multiple disordered regions and RNA-binding domains that contribute to different protein functions. P keeps N soluble after expression to allow a concerted binding of N to the viral RNA. This results in the encapsidation of the viral genome by N, while P acts additionally as a cofactor for the viral polymerase, enabling viral transcription and replication. Here, we will review the formation and function of those viral inclusion bodies upon infection with NSVs with respect to their nature as biomolecular condensates.https://www.mdpi.com/2073-4409/10/6/1460negative strand RNA viruses (NSV)viral inclusion bodiesbiomolecular condensatesliquid-liquid phase separation (LLPS)viral replicationnucleoprotein
collection DOAJ
language English
format Article
sources DOAJ
author Olga Dolnik
Gesche K. Gerresheim
Nadine Biedenkopf
spellingShingle Olga Dolnik
Gesche K. Gerresheim
Nadine Biedenkopf
New Perspectives on the Biogenesis of Viral Inclusion Bodies in Negative-Sense RNA Virus Infections
Cells
negative strand RNA viruses (NSV)
viral inclusion bodies
biomolecular condensates
liquid-liquid phase separation (LLPS)
viral replication
nucleoprotein
author_facet Olga Dolnik
Gesche K. Gerresheim
Nadine Biedenkopf
author_sort Olga Dolnik
title New Perspectives on the Biogenesis of Viral Inclusion Bodies in Negative-Sense RNA Virus Infections
title_short New Perspectives on the Biogenesis of Viral Inclusion Bodies in Negative-Sense RNA Virus Infections
title_full New Perspectives on the Biogenesis of Viral Inclusion Bodies in Negative-Sense RNA Virus Infections
title_fullStr New Perspectives on the Biogenesis of Viral Inclusion Bodies in Negative-Sense RNA Virus Infections
title_full_unstemmed New Perspectives on the Biogenesis of Viral Inclusion Bodies in Negative-Sense RNA Virus Infections
title_sort new perspectives on the biogenesis of viral inclusion bodies in negative-sense rna virus infections
publisher MDPI AG
series Cells
issn 2073-4409
publishDate 2021-06-01
description Infections by negative strand RNA viruses (NSVs) induce the formation of viral inclusion bodies (IBs) in the host cell that segregate viral as well as cellular proteins to enable efficient viral replication. The induction of those membrane-less viral compartments leads inevitably to structural remodeling of the cellular architecture. Recent studies suggested that viral IBs have properties of biomolecular condensates (or liquid organelles), as have previously been shown for other membrane-less cellular compartments like stress granules or P-bodies. Biomolecular condensates are highly dynamic structures formed by liquid-liquid phase separation (LLPS). Key drivers for LLPS in cells are multivalent protein:protein and protein:RNA interactions leading to specialized areas in the cell that recruit molecules with similar properties, while other non-similar molecules are excluded. These typical features of cellular biomolecular condensates are also a common characteristic in the biogenesis of viral inclusion bodies. Viral IBs are predominantly induced by the expression of the viral nucleoprotein (N, NP) and phosphoprotein (P); both are characterized by a special protein architecture containing multiple disordered regions and RNA-binding domains that contribute to different protein functions. P keeps N soluble after expression to allow a concerted binding of N to the viral RNA. This results in the encapsidation of the viral genome by N, while P acts additionally as a cofactor for the viral polymerase, enabling viral transcription and replication. Here, we will review the formation and function of those viral inclusion bodies upon infection with NSVs with respect to their nature as biomolecular condensates.
topic negative strand RNA viruses (NSV)
viral inclusion bodies
biomolecular condensates
liquid-liquid phase separation (LLPS)
viral replication
nucleoprotein
url https://www.mdpi.com/2073-4409/10/6/1460
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