SIV vpx is essential for macrophage infection but not for development of AIDS.

Analysis of rhesus macaques infected with a vpx deletion mutant virus of simian immunodeficiency virus mac239 (SIVΔvpx) demonstrates that Vpx is essential for efficient monocyte/macrophage infection in vivo but is not necessary for development of AIDS. To compare myeloid-lineage cell infection in mo...

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Main Authors: Susan V Westmoreland, A Peter Converse, Kasia Hrecka, Mollie Hurley, Heather Knight, Michael Piatak, Jeffrey Lifson, Keith G Mansfield, Jacek Skowronski, Ronald C Desrosiers
Format: Article
Language:English
Published: Public Library of Science (PLoS) 2014-01-01
Series:PLoS ONE
Online Access:http://europepmc.org/articles/PMC3897363?pdf=render
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spelling doaj-7d79461adfa943c09a703f3e6947b0212020-11-25T01:42:56ZengPublic Library of Science (PLoS)PLoS ONE1932-62032014-01-0191e8446310.1371/journal.pone.0084463SIV vpx is essential for macrophage infection but not for development of AIDS.Susan V WestmorelandA Peter ConverseKasia HreckaMollie HurleyHeather KnightMichael PiatakJeffrey LifsonKeith G MansfieldJacek SkowronskiRonald C DesrosiersAnalysis of rhesus macaques infected with a vpx deletion mutant virus of simian immunodeficiency virus mac239 (SIVΔvpx) demonstrates that Vpx is essential for efficient monocyte/macrophage infection in vivo but is not necessary for development of AIDS. To compare myeloid-lineage cell infection in monkeys infected with SIVΔvpx compared to SIVmac239, we analyzed lymphoid and gastrointestinal tissues from SIVΔvpx-infected rhesus (n = 5), SIVmac239-infected rhesus with SIV encephalitis (7 SIV239E), those without encephalitis (4 SIV239noE), and other SIV mutant viruses with low viral loads (4 SIVΔnef, 2 SIVΔ3). SIV+ macrophages and the percentage of total SIV+ cells that were macrophages in spleen and lymph nodes were significantly lower in rhesus infected with SIVΔvpx (2.2%) compared to those infected with SIV239E (22.7%), SIV239noE (8.2%), and SIV mutant viruses (10.1%). In colon, SIVΔvpx monkeys had fewer SIV+ cells, no SIV+ macrophages, and lower percentage of SIV+ cells that were macrophages than the other 3 groups. Only 2 SIVΔvpx monkeys exhibited detectable virus in the colon. We demonstrate that Vpx is essential for efficient macrophage infection in vivo and that simian AIDS and death can occur in the absence of detectable macrophage infection.http://europepmc.org/articles/PMC3897363?pdf=render
collection DOAJ
language English
format Article
sources DOAJ
author Susan V Westmoreland
A Peter Converse
Kasia Hrecka
Mollie Hurley
Heather Knight
Michael Piatak
Jeffrey Lifson
Keith G Mansfield
Jacek Skowronski
Ronald C Desrosiers
spellingShingle Susan V Westmoreland
A Peter Converse
Kasia Hrecka
Mollie Hurley
Heather Knight
Michael Piatak
Jeffrey Lifson
Keith G Mansfield
Jacek Skowronski
Ronald C Desrosiers
SIV vpx is essential for macrophage infection but not for development of AIDS.
PLoS ONE
author_facet Susan V Westmoreland
A Peter Converse
Kasia Hrecka
Mollie Hurley
Heather Knight
Michael Piatak
Jeffrey Lifson
Keith G Mansfield
Jacek Skowronski
Ronald C Desrosiers
author_sort Susan V Westmoreland
title SIV vpx is essential for macrophage infection but not for development of AIDS.
title_short SIV vpx is essential for macrophage infection but not for development of AIDS.
title_full SIV vpx is essential for macrophage infection but not for development of AIDS.
title_fullStr SIV vpx is essential for macrophage infection but not for development of AIDS.
title_full_unstemmed SIV vpx is essential for macrophage infection but not for development of AIDS.
title_sort siv vpx is essential for macrophage infection but not for development of aids.
publisher Public Library of Science (PLoS)
series PLoS ONE
issn 1932-6203
publishDate 2014-01-01
description Analysis of rhesus macaques infected with a vpx deletion mutant virus of simian immunodeficiency virus mac239 (SIVΔvpx) demonstrates that Vpx is essential for efficient monocyte/macrophage infection in vivo but is not necessary for development of AIDS. To compare myeloid-lineage cell infection in monkeys infected with SIVΔvpx compared to SIVmac239, we analyzed lymphoid and gastrointestinal tissues from SIVΔvpx-infected rhesus (n = 5), SIVmac239-infected rhesus with SIV encephalitis (7 SIV239E), those without encephalitis (4 SIV239noE), and other SIV mutant viruses with low viral loads (4 SIVΔnef, 2 SIVΔ3). SIV+ macrophages and the percentage of total SIV+ cells that were macrophages in spleen and lymph nodes were significantly lower in rhesus infected with SIVΔvpx (2.2%) compared to those infected with SIV239E (22.7%), SIV239noE (8.2%), and SIV mutant viruses (10.1%). In colon, SIVΔvpx monkeys had fewer SIV+ cells, no SIV+ macrophages, and lower percentage of SIV+ cells that were macrophages than the other 3 groups. Only 2 SIVΔvpx monkeys exhibited detectable virus in the colon. We demonstrate that Vpx is essential for efficient macrophage infection in vivo and that simian AIDS and death can occur in the absence of detectable macrophage infection.
url http://europepmc.org/articles/PMC3897363?pdf=render
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