Cellular N-myristoyltransferases play a crucial picornavirus genus-specific role in viral assembly, virion maturation, and infectivity

In nearly all picornaviruses the precursor of the smallest capsid protein VP4 undergoes co-translational N-terminal myristoylation by host cell N-myristoyltransferases (NMTs). Curtailing this modification by mutation of the myristoylation signal in poliovirus has been shown to result in severe assem...

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Autores principales: Corbic Ramljak, Irena, Stanger, Julia, Real-Hohn, Antonio, Dreier, Dominik, Wimmer, Laurin, Redlberger-Fritz, Monika, Fischl, Wolfgang, Klingel, Karin, Mihovilovic, Marko D., Blaas, Dieter, Kowalski, Heinrich
Formato: Online Artículo Texto
Lenguaje:English
Publicado: Public Library of Science 2018
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Research Article
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC6089459/
https://www.ncbi.nlm.nih.gov/pubmed/30080883
http://dx.doi.org/10.1371/journal.ppat.1007203
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author Corbic Ramljak, Irena
Stanger, Julia
Real-Hohn, Antonio
Dreier, Dominik
Wimmer, Laurin
Redlberger-Fritz, Monika
Fischl, Wolfgang
Klingel, Karin
Mihovilovic, Marko D.
Blaas, Dieter
Kowalski, Heinrich
author_facet Corbic Ramljak, Irena
Stanger, Julia
Real-Hohn, Antonio
Dreier, Dominik
Wimmer, Laurin
Redlberger-Fritz, Monika
Fischl, Wolfgang
Klingel, Karin
Mihovilovic, Marko D.
Blaas, Dieter
Kowalski, Heinrich
author_sort Corbic Ramljak, Irena
collection PubMed
description In nearly all picornaviruses the precursor of the smallest capsid protein VP4 undergoes co-translational N-terminal myristoylation by host cell N-myristoyltransferases (NMTs). Curtailing this modification by mutation of the myristoylation signal in poliovirus has been shown to result in severe assembly defects and very little, if any, progeny virus production. Avoiding possible pleiotropic effects of such mutations, we here used pharmacological abrogation of myristoylation with the NMT inhibitor DDD85646, a pyrazole sulfonamide originally developed against trypanosomal NMT. Infection of HeLa cells with coxsackievirus B3 in the presence of this drug decreased VP0 acylation at least 100-fold, resulting in a defect both early and late in virus morphogenesis, which diminishes the yield of viral progeny by about 90%. Virus particles still produced consisted mainly of provirions containing RNA and uncleaved VP0 and, to a substantially lesser extent, of mature virions with cleaved VP0. This indicates an important role of myristoylation in the viral maturation cleavage. By electron microscopy, these RNA-filled particles were indistinguishable from virus produced under control conditions. Nevertheless, their specific infectivity decreased by about five hundred fold. Since host cell-attachment was not markedly impaired, their defect must lie in the inability to transfer their genomic RNA into the cytosol, likely at the level of endosomal pore formation. Strikingly, neither parechoviruses nor kobuviruses are affected by DDD85646, which appears to correlate with their native capsid containing only unprocessed VP0. Individual knockout of the genes encoding the two human NMT isozymes in haploid HAP1 cells further demonstrated the pivotal role for HsNMT1, with little contribution by HsNMT2, in the virus replication cycle. Our results also indicate that inhibition of NMT can possibly be exploited for controlling the infection by a wide spectrum of picornaviruses.
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spelling pubmed-60894592018-08-30 Cellular N-myristoyltransferases play a crucial picornavirus genus-specific role in viral assembly, virion maturation, and infectivity Corbic Ramljak, Irena Stanger, Julia Real-Hohn, Antonio Dreier, Dominik Wimmer, Laurin Redlberger-Fritz, Monika Fischl, Wolfgang Klingel, Karin Mihovilovic, Marko D. Blaas, Dieter Kowalski, Heinrich PLoS Pathog Research Article In nearly all picornaviruses the precursor of the smallest capsid protein VP4 undergoes co-translational N-terminal myristoylation by host cell N-myristoyltransferases (NMTs). Curtailing this modification by mutation of the myristoylation signal in poliovirus has been shown to result in severe assembly defects and very little, if any, progeny virus production. Avoiding possible pleiotropic effects of such mutations, we here used pharmacological abrogation of myristoylation with the NMT inhibitor DDD85646, a pyrazole sulfonamide originally developed against trypanosomal NMT. Infection of HeLa cells with coxsackievirus B3 in the presence of this drug decreased VP0 acylation at least 100-fold, resulting in a defect both early and late in virus morphogenesis, which diminishes the yield of viral progeny by about 90%. Virus particles still produced consisted mainly of provirions containing RNA and uncleaved VP0 and, to a substantially lesser extent, of mature virions with cleaved VP0. This indicates an important role of myristoylation in the viral maturation cleavage. By electron microscopy, these RNA-filled particles were indistinguishable from virus produced under control conditions. Nevertheless, their specific infectivity decreased by about five hundred fold. Since host cell-attachment was not markedly impaired, their defect must lie in the inability to transfer their genomic RNA into the cytosol, likely at the level of endosomal pore formation. Strikingly, neither parechoviruses nor kobuviruses are affected by DDD85646, which appears to correlate with their native capsid containing only unprocessed VP0. Individual knockout of the genes encoding the two human NMT isozymes in haploid HAP1 cells further demonstrated the pivotal role for HsNMT1, with little contribution by HsNMT2, in the virus replication cycle. Our results also indicate that inhibition of NMT can possibly be exploited for controlling the infection by a wide spectrum of picornaviruses. Public Library of Science 2018-08-06 /pmc/articles/PMC6089459/ /pubmed/30080883 http://dx.doi.org/10.1371/journal.ppat.1007203 Text en © 2018 Ramljak et al http://creativecommons.org/licenses/by/4.0/ This is an open access article distributed under the terms of the Creative Commons Attribution License (http://creativecommons.org/licenses/by/4.0/) , which permits unrestricted use, distribution, and reproduction in any medium, provided the original author and source are credited.
spellingShingle Research Article
Corbic Ramljak, Irena
Stanger, Julia
Real-Hohn, Antonio
Dreier, Dominik
Wimmer, Laurin
Redlberger-Fritz, Monika
Fischl, Wolfgang
Klingel, Karin
Mihovilovic, Marko D.
Blaas, Dieter
Kowalski, Heinrich
Cellular N-myristoyltransferases play a crucial picornavirus genus-specific role in viral assembly, virion maturation, and infectivity
title Cellular N-myristoyltransferases play a crucial picornavirus genus-specific role in viral assembly, virion maturation, and infectivity
title_full Cellular N-myristoyltransferases play a crucial picornavirus genus-specific role in viral assembly, virion maturation, and infectivity
title_fullStr Cellular N-myristoyltransferases play a crucial picornavirus genus-specific role in viral assembly, virion maturation, and infectivity
title_full_unstemmed Cellular N-myristoyltransferases play a crucial picornavirus genus-specific role in viral assembly, virion maturation, and infectivity
title_short Cellular N-myristoyltransferases play a crucial picornavirus genus-specific role in viral assembly, virion maturation, and infectivity
title_sort cellular n-myristoyltransferases play a crucial picornavirus genus-specific role in viral assembly, virion maturation, and infectivity
topic Research Article
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC6089459/
https://www.ncbi.nlm.nih.gov/pubmed/30080883
http://dx.doi.org/10.1371/journal.ppat.1007203
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