Natural selection differences detected in key protein domains between non-pathogenic and pathogenic Feline Coronavirus phenotypes

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Feline Coronaviruses (FCoVs) commonly cause mild enteric infections in felines worldwide (termed Feline Enteric Coronavirus [FECV]), with around 12% developing into deadly Feline Infectious Peritonitis (FIP; Feline Infectious Peritonitis Virus [FIPV]). Genomic differences between FECV and FIPV have...

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Autores principales: Zehr, Jordan D., Pond, Sergei L. Kosakovsky, Millet, Jean K., Olarte-Castillo, Ximena A., Lucaci, Alexander G., Shank, Stephen D., Ceres, Kristina M., Choi, Annette, Whittaker, Gary R., Goodman, Laura B., Stanhope, Michael J.
Formato: Online Artículo Texto
Lenguaje:English
Publicado: Cold Spring Harbor Laboratory 2023
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Article
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC9882035/
https://www.ncbi.nlm.nih.gov/pubmed/36712007
http://dx.doi.org/10.1101/2023.01.11.523607
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author Zehr, Jordan D.
Pond, Sergei L. Kosakovsky
Millet, Jean K.
Olarte-Castillo, Ximena A.
Lucaci, Alexander G.
Shank, Stephen D.
Ceres, Kristina M.
Choi, Annette
Whittaker, Gary R.
Goodman, Laura B.
Stanhope, Michael J.
author_facet Zehr, Jordan D.
Pond, Sergei L. Kosakovsky
Millet, Jean K.
Olarte-Castillo, Ximena A.
Lucaci, Alexander G.
Shank, Stephen D.
Ceres, Kristina M.
Choi, Annette
Whittaker, Gary R.
Goodman, Laura B.
Stanhope, Michael J.
author_sort Zehr, Jordan D.
collection PubMed
description Feline Coronaviruses (FCoVs) commonly cause mild enteric infections in felines worldwide (termed Feline Enteric Coronavirus [FECV]), with around 12% developing into deadly Feline Infectious Peritonitis (FIP; Feline Infectious Peritonitis Virus [FIPV]). Genomic differences between FECV and FIPV have been reported, yet the putative genotypic basis of the highly pathogenic phenotype remains unclear. Here, we used state-of-the-art molecular evolutionary genetic statistical techniques to identify and compare differences in natural selection pressure between FECV and FIPV sequences, as well as to identify FIPV and FECV specific signals of positive selection. We analyzed full length FCoV protein coding genes thought to contain mutations associated with FIPV (Spike, ORF3abc, and ORF7ab). We identified two sites exhibiting differences in natural selection pressure between FECV and FIPV: one within the S1/S2 furin cleavage site, and the other within the fusion domain of Spike. We also found 15 sites subject to positive selection associated with FIPV within Spike, 11 of which have not previously been suggested as possibly relevant to FIP development. These sites fall within Spike protein subdomains that participate in host cell receptor interaction, immune evasion, tropism shifts, host cellular entry, and viral escape. There were 14 sites (12 novel) within Spike under positive selection associated with the FECV phenotype, almost exclusively within the S1/S2 furin cleavage site and adjacent C domain, along with a signal of relaxed selection in FIPV relative to FECV, suggesting that furin cleavage functionality may not be needed for FIPV. Positive selection inferred in ORF7b was associated with the FECV phenotype, and included 24 positively selected sites, while ORF7b had signals of relaxed selection in FIPV. We found evidence of positive selection in ORF3c in FCoV wide analyses, but no specific association with the FIPV or FECV phenotype. We hypothesize that some combination of mutations in FECV may contribute to FIP development, and that is unlikely to be one singular “switch” mutational event. This work expands our understanding of the complexities of FIP development and provides insights into how evolutionary forces may alter pathogenesis in coronavirus genomes.
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spelling pubmed-98820352023-01-28 Natural selection differences detected in key protein domains between non-pathogenic and pathogenic Feline Coronavirus phenotypes Zehr, Jordan D. Pond, Sergei L. Kosakovsky Millet, Jean K. Olarte-Castillo, Ximena A. Lucaci, Alexander G. Shank, Stephen D. Ceres, Kristina M. Choi, Annette Whittaker, Gary R. Goodman, Laura B. Stanhope, Michael J. bioRxiv Article Feline Coronaviruses (FCoVs) commonly cause mild enteric infections in felines worldwide (termed Feline Enteric Coronavirus [FECV]), with around 12% developing into deadly Feline Infectious Peritonitis (FIP; Feline Infectious Peritonitis Virus [FIPV]). Genomic differences between FECV and FIPV have been reported, yet the putative genotypic basis of the highly pathogenic phenotype remains unclear. Here, we used state-of-the-art molecular evolutionary genetic statistical techniques to identify and compare differences in natural selection pressure between FECV and FIPV sequences, as well as to identify FIPV and FECV specific signals of positive selection. We analyzed full length FCoV protein coding genes thought to contain mutations associated with FIPV (Spike, ORF3abc, and ORF7ab). We identified two sites exhibiting differences in natural selection pressure between FECV and FIPV: one within the S1/S2 furin cleavage site, and the other within the fusion domain of Spike. We also found 15 sites subject to positive selection associated with FIPV within Spike, 11 of which have not previously been suggested as possibly relevant to FIP development. These sites fall within Spike protein subdomains that participate in host cell receptor interaction, immune evasion, tropism shifts, host cellular entry, and viral escape. There were 14 sites (12 novel) within Spike under positive selection associated with the FECV phenotype, almost exclusively within the S1/S2 furin cleavage site and adjacent C domain, along with a signal of relaxed selection in FIPV relative to FECV, suggesting that furin cleavage functionality may not be needed for FIPV. Positive selection inferred in ORF7b was associated with the FECV phenotype, and included 24 positively selected sites, while ORF7b had signals of relaxed selection in FIPV. We found evidence of positive selection in ORF3c in FCoV wide analyses, but no specific association with the FIPV or FECV phenotype. We hypothesize that some combination of mutations in FECV may contribute to FIP development, and that is unlikely to be one singular “switch” mutational event. This work expands our understanding of the complexities of FIP development and provides insights into how evolutionary forces may alter pathogenesis in coronavirus genomes. Cold Spring Harbor Laboratory 2023-01-11 /pmc/articles/PMC9882035/ /pubmed/36712007 http://dx.doi.org/10.1101/2023.01.11.523607 Text en https://creativecommons.org/licenses/by-nc-nd/4.0/This work is licensed under a Creative Commons Attribution-NonCommercial-NoDerivatives 4.0 International License (https://creativecommons.org/licenses/by-nc-nd/4.0/) , which allows reusers to copy and distribute the material in any medium or format in unadapted form only, for noncommercial purposes only, and only so long as attribution is given to the creator.
spellingShingle Article
Zehr, Jordan D.
Pond, Sergei L. Kosakovsky
Millet, Jean K.
Olarte-Castillo, Ximena A.
Lucaci, Alexander G.
Shank, Stephen D.
Ceres, Kristina M.
Choi, Annette
Whittaker, Gary R.
Goodman, Laura B.
Stanhope, Michael J.
Natural selection differences detected in key protein domains between non-pathogenic and pathogenic Feline Coronavirus phenotypes
title Natural selection differences detected in key protein domains between non-pathogenic and pathogenic Feline Coronavirus phenotypes
title_full Natural selection differences detected in key protein domains between non-pathogenic and pathogenic Feline Coronavirus phenotypes
title_fullStr Natural selection differences detected in key protein domains between non-pathogenic and pathogenic Feline Coronavirus phenotypes
title_full_unstemmed Natural selection differences detected in key protein domains between non-pathogenic and pathogenic Feline Coronavirus phenotypes
title_short Natural selection differences detected in key protein domains between non-pathogenic and pathogenic Feline Coronavirus phenotypes
title_sort natural selection differences detected in key protein domains between non-pathogenic and pathogenic feline coronavirus phenotypes
topic Article
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC9882035/
https://www.ncbi.nlm.nih.gov/pubmed/36712007
http://dx.doi.org/10.1101/2023.01.11.523607
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