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Subclinical Infection of Macaques and Baboons with A Baboon Simarterivirus

Simarteriviruses (Arteriviridae: Simarterivirinae) are commonly found at high titers in the blood of African monkeys but do not cause overt disease in these hosts. In contrast, simarteriviruses cause severe disease in Asian macaques upon accidental or experimental transmission. Here, we sought to be...

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Autores principales: Buechler, Connor R., Semler, Matthew, Baker, David A., Newman, Christina, Cornish, Joseph P., Chavez, Deborah, Guerra, Bernadette, Lanford, Robert, Brasky, Kathy, Kuhn, Jens H., Johnson, Reed F., O’Connor, David H., Bailey, Adam L.
Formato: Online Artículo Texto
Lenguaje:English
Publicado: MDPI 2018
Materias:
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC6316555/
https://www.ncbi.nlm.nih.gov/pubmed/30544677
http://dx.doi.org/10.3390/v10120701
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author Buechler, Connor R.
Semler, Matthew
Baker, David A.
Newman, Christina
Cornish, Joseph P.
Chavez, Deborah
Guerra, Bernadette
Lanford, Robert
Brasky, Kathy
Kuhn, Jens H.
Johnson, Reed F.
O’Connor, David H.
Bailey, Adam L.
author_facet Buechler, Connor R.
Semler, Matthew
Baker, David A.
Newman, Christina
Cornish, Joseph P.
Chavez, Deborah
Guerra, Bernadette
Lanford, Robert
Brasky, Kathy
Kuhn, Jens H.
Johnson, Reed F.
O’Connor, David H.
Bailey, Adam L.
author_sort Buechler, Connor R.
collection PubMed
description Simarteriviruses (Arteriviridae: Simarterivirinae) are commonly found at high titers in the blood of African monkeys but do not cause overt disease in these hosts. In contrast, simarteriviruses cause severe disease in Asian macaques upon accidental or experimental transmission. Here, we sought to better understand the host-dependent drivers of simarterivirus pathogenesis by infecting olive baboons (n = 4) and rhesus monkeys (n = 4) with the simarterivirus Southwest baboon virus 1 (SWBV-1). Surprisingly, none of the animals in our study showed signs of disease following SWBV-1 inoculation. Three animals (two rhesus monkeys and one olive baboon) became infected and sustained high levels of SWBV-1 viremia for the duration of the study. The course of SWBV-1 infection was highly predictable: plasma viremia peaked between 1 × 10(7) and 1 × 10(8) vRNA copies/mL at 3–10 days post-inoculation, which was followed by a relative nadir and then establishment of a stable set-point between 1 × 10(6) and 1 × 10(7) vRNA copies/mL for the remainder of the study (56 days). We characterized cellular and antibody responses to SWBV-1 infection in these animals, demonstrating that macaques and baboons mount similar responses to SWBV-1 infection, yet these responses are ineffective at clearing SWBV-1 infection. SWBV-1 sequencing revealed the accumulation of non-synonymous mutations in a region of the genome that corresponds to an immunodominant epitope in the simarterivirus major envelope glycoprotein GP5, which likely contribute to viral persistence by enabling escape from host antibodies.
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spelling pubmed-63165552019-01-10 Subclinical Infection of Macaques and Baboons with A Baboon Simarterivirus Buechler, Connor R. Semler, Matthew Baker, David A. Newman, Christina Cornish, Joseph P. Chavez, Deborah Guerra, Bernadette Lanford, Robert Brasky, Kathy Kuhn, Jens H. Johnson, Reed F. O’Connor, David H. Bailey, Adam L. Viruses Article Simarteriviruses (Arteriviridae: Simarterivirinae) are commonly found at high titers in the blood of African monkeys but do not cause overt disease in these hosts. In contrast, simarteriviruses cause severe disease in Asian macaques upon accidental or experimental transmission. Here, we sought to better understand the host-dependent drivers of simarterivirus pathogenesis by infecting olive baboons (n = 4) and rhesus monkeys (n = 4) with the simarterivirus Southwest baboon virus 1 (SWBV-1). Surprisingly, none of the animals in our study showed signs of disease following SWBV-1 inoculation. Three animals (two rhesus monkeys and one olive baboon) became infected and sustained high levels of SWBV-1 viremia for the duration of the study. The course of SWBV-1 infection was highly predictable: plasma viremia peaked between 1 × 10(7) and 1 × 10(8) vRNA copies/mL at 3–10 days post-inoculation, which was followed by a relative nadir and then establishment of a stable set-point between 1 × 10(6) and 1 × 10(7) vRNA copies/mL for the remainder of the study (56 days). We characterized cellular and antibody responses to SWBV-1 infection in these animals, demonstrating that macaques and baboons mount similar responses to SWBV-1 infection, yet these responses are ineffective at clearing SWBV-1 infection. SWBV-1 sequencing revealed the accumulation of non-synonymous mutations in a region of the genome that corresponds to an immunodominant epitope in the simarterivirus major envelope glycoprotein GP5, which likely contribute to viral persistence by enabling escape from host antibodies. MDPI 2018-12-10 /pmc/articles/PMC6316555/ /pubmed/30544677 http://dx.doi.org/10.3390/v10120701 Text en © 2018 by the authors. Licensee MDPI, Basel, Switzerland. This article is an open access article distributed under the terms and conditions of the Creative Commons Attribution (CC BY) license (http://creativecommons.org/licenses/by/4.0/).
spellingShingle Article
Buechler, Connor R.
Semler, Matthew
Baker, David A.
Newman, Christina
Cornish, Joseph P.
Chavez, Deborah
Guerra, Bernadette
Lanford, Robert
Brasky, Kathy
Kuhn, Jens H.
Johnson, Reed F.
O’Connor, David H.
Bailey, Adam L.
Subclinical Infection of Macaques and Baboons with A Baboon Simarterivirus
title Subclinical Infection of Macaques and Baboons with A Baboon Simarterivirus
title_full Subclinical Infection of Macaques and Baboons with A Baboon Simarterivirus
title_fullStr Subclinical Infection of Macaques and Baboons with A Baboon Simarterivirus
title_full_unstemmed Subclinical Infection of Macaques and Baboons with A Baboon Simarterivirus
title_short Subclinical Infection of Macaques and Baboons with A Baboon Simarterivirus
title_sort subclinical infection of macaques and baboons with a baboon simarterivirus
topic Article
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC6316555/
https://www.ncbi.nlm.nih.gov/pubmed/30544677
http://dx.doi.org/10.3390/v10120701
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