Molecular modelling of the HCMV IL-10 protein isoforms and analysis of their interaction with the human IL-10 receptor

The human cytomegalovirus (HCMV) UL111A gene encodes several homologs of the cellular interleukin 10 (cIL-10). Alternative splicing in the UL111A region produces two relatively well-characterized transcripts designated cmvIL-10 (isoform A) and LAcmvIL-10 (isoform B). The cmvIL-10 protein is the best...

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Autores principales: Pantaleão, Simone Queiroz, Camillo, Lívia de Moraes Bomediano, Neves, Tainan Cerqueira, Menezes, Isabela de Godoy, Stangherlin, Lucas Matheus, Batista, Helena Beatriz de Carvalho Ruthner, Poole, Emma, Nevels, Michael, Philot, Eric Alisson, Scott, Ana Ligia, Carlan da Silva, Maria Cristina
Formato: Online Artículo Texto
Lenguaje:English
Publicado: Public Library of Science 2022
Materias:
Research Article
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC9704672/
https://www.ncbi.nlm.nih.gov/pubmed/36441804
http://dx.doi.org/10.1371/journal.pone.0277953
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author Pantaleão, Simone Queiroz
Camillo, Lívia de Moraes Bomediano
Neves, Tainan Cerqueira
Menezes, Isabela de Godoy
Stangherlin, Lucas Matheus
Batista, Helena Beatriz de Carvalho Ruthner
Poole, Emma
Nevels, Michael
Philot, Eric Alisson
Scott, Ana Ligia
Carlan da Silva, Maria Cristina
author_facet Pantaleão, Simone Queiroz
Camillo, Lívia de Moraes Bomediano
Neves, Tainan Cerqueira
Menezes, Isabela de Godoy
Stangherlin, Lucas Matheus
Batista, Helena Beatriz de Carvalho Ruthner
Poole, Emma
Nevels, Michael
Philot, Eric Alisson
Scott, Ana Ligia
Carlan da Silva, Maria Cristina
author_sort Pantaleão, Simone Queiroz
collection PubMed
description The human cytomegalovirus (HCMV) UL111A gene encodes several homologs of the cellular interleukin 10 (cIL-10). Alternative splicing in the UL111A region produces two relatively well-characterized transcripts designated cmvIL-10 (isoform A) and LAcmvIL-10 (isoform B). The cmvIL-10 protein is the best characterized, both structurally and functionally, and has many immunosuppressive activities similar to cIL-10, while LAcmvIL-10 has more restricted biological activities. Alternative splicing also results in five less studied UL111A transcripts encoding additional proteins homologous to cIL-10 (isoforms C to G). These transcripts were identified during productive HCMV infection of MRC-5 cells with the high passage laboratory adapted AD169 strain, and the structure and properties of the corresponding proteins are largely unknown. Moreover, it is unclear whether these protein isoforms are able to bind the cellular IL-10 receptor and induce signalling. In the present study, we investigated the expression spectrum of UL111A transcripts in fully permissive MRC-5 cells and semi permissive U251 cells infected with the low passage HCMV strain TB40E. We identified a new spliced transcript (H) expressed during productive infection. Using computational methods, we carried out molecular modelling studies on the three-dimensional structures of the HCMV IL-10 proteins encoded by the transcripts detected in our work (cmvIL-10 (A), LAcmvIL-10 (B), E, F and H) and on their interaction with the human IL-10 receptor (IL-10R1). The modelling predicts clear differences between the isoform structures. Furthermore, the in silico simulations (molecular dynamics simulation and normal-mode analyses) allowed us to evaluate regions that contain potential receptor binding sites in each isoform. The analyses demonstrate that the complexes between the isoforms and IL-10R1 present different types of molecular interactions and consequently different affinities and stabilities. The knowledge about structure and expression of specific viral IL-10 isoforms has implications for understanding of their properties and role in HCMV immune evasion and pathogenesis.
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spelling pubmed-97046722022-11-29 Molecular modelling of the HCMV IL-10 protein isoforms and analysis of their interaction with the human IL-10 receptor Pantaleão, Simone Queiroz Camillo, Lívia de Moraes Bomediano Neves, Tainan Cerqueira Menezes, Isabela de Godoy Stangherlin, Lucas Matheus Batista, Helena Beatriz de Carvalho Ruthner Poole, Emma Nevels, Michael Philot, Eric Alisson Scott, Ana Ligia Carlan da Silva, Maria Cristina PLoS One Research Article The human cytomegalovirus (HCMV) UL111A gene encodes several homologs of the cellular interleukin 10 (cIL-10). Alternative splicing in the UL111A region produces two relatively well-characterized transcripts designated cmvIL-10 (isoform A) and LAcmvIL-10 (isoform B). The cmvIL-10 protein is the best characterized, both structurally and functionally, and has many immunosuppressive activities similar to cIL-10, while LAcmvIL-10 has more restricted biological activities. Alternative splicing also results in five less studied UL111A transcripts encoding additional proteins homologous to cIL-10 (isoforms C to G). These transcripts were identified during productive HCMV infection of MRC-5 cells with the high passage laboratory adapted AD169 strain, and the structure and properties of the corresponding proteins are largely unknown. Moreover, it is unclear whether these protein isoforms are able to bind the cellular IL-10 receptor and induce signalling. In the present study, we investigated the expression spectrum of UL111A transcripts in fully permissive MRC-5 cells and semi permissive U251 cells infected with the low passage HCMV strain TB40E. We identified a new spliced transcript (H) expressed during productive infection. Using computational methods, we carried out molecular modelling studies on the three-dimensional structures of the HCMV IL-10 proteins encoded by the transcripts detected in our work (cmvIL-10 (A), LAcmvIL-10 (B), E, F and H) and on their interaction with the human IL-10 receptor (IL-10R1). The modelling predicts clear differences between the isoform structures. Furthermore, the in silico simulations (molecular dynamics simulation and normal-mode analyses) allowed us to evaluate regions that contain potential receptor binding sites in each isoform. The analyses demonstrate that the complexes between the isoforms and IL-10R1 present different types of molecular interactions and consequently different affinities and stabilities. The knowledge about structure and expression of specific viral IL-10 isoforms has implications for understanding of their properties and role in HCMV immune evasion and pathogenesis. Public Library of Science 2022-11-28 /pmc/articles/PMC9704672/ /pubmed/36441804 http://dx.doi.org/10.1371/journal.pone.0277953 Text en © 2022 Pantaleão et al https://creativecommons.org/licenses/by/4.0/This is an open access article distributed under the terms of the Creative Commons Attribution License (https://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
Pantaleão, Simone Queiroz
Camillo, Lívia de Moraes Bomediano
Neves, Tainan Cerqueira
Menezes, Isabela de Godoy
Stangherlin, Lucas Matheus
Batista, Helena Beatriz de Carvalho Ruthner
Poole, Emma
Nevels, Michael
Philot, Eric Alisson
Scott, Ana Ligia
Carlan da Silva, Maria Cristina
Molecular modelling of the HCMV IL-10 protein isoforms and analysis of their interaction with the human IL-10 receptor
title Molecular modelling of the HCMV IL-10 protein isoforms and analysis of their interaction with the human IL-10 receptor
title_full Molecular modelling of the HCMV IL-10 protein isoforms and analysis of their interaction with the human IL-10 receptor
title_fullStr Molecular modelling of the HCMV IL-10 protein isoforms and analysis of their interaction with the human IL-10 receptor
title_full_unstemmed Molecular modelling of the HCMV IL-10 protein isoforms and analysis of their interaction with the human IL-10 receptor
title_short Molecular modelling of the HCMV IL-10 protein isoforms and analysis of their interaction with the human IL-10 receptor
title_sort molecular modelling of the hcmv il-10 protein isoforms and analysis of their interaction with the human il-10 receptor
topic Research Article
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC9704672/
https://www.ncbi.nlm.nih.gov/pubmed/36441804
http://dx.doi.org/10.1371/journal.pone.0277953
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