Productive Replication of HIV-1 but Not SIVmac in Small Ruminant Cells

Animal lentiviruses (LVs) have been proven to have the capacity to cross the species barrier, to adapt in the new hosts, and to increase their pathogenesis, therefore leading to the emergence of threatening diseases. However, their potential for widespread diffusion is limited by restrictive cellula...

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Autores principales: Chergui, Hibet Errahmane, Idres, Takfarinas, Chaudesaigues, Chloé, Noueihed, Diana, Gagnon, Jean, Chebloune, Yahia
Formato: Online Artículo Texto
Lenguaje:English
Publicado: MDPI 2022
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Article
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC9316499/
https://www.ncbi.nlm.nih.gov/pubmed/35890043
http://dx.doi.org/10.3390/pathogens11070799
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author Chergui, Hibet Errahmane
Idres, Takfarinas
Chaudesaigues, Chloé
Noueihed, Diana
Gagnon, Jean
Chebloune, Yahia
author_facet Chergui, Hibet Errahmane
Idres, Takfarinas
Chaudesaigues, Chloé
Noueihed, Diana
Gagnon, Jean
Chebloune, Yahia
author_sort Chergui, Hibet Errahmane
collection PubMed
description Animal lentiviruses (LVs) have been proven to have the capacity to cross the species barrier, to adapt in the new hosts, and to increase their pathogenesis, therefore leading to the emergence of threatening diseases. However, their potential for widespread diffusion is limited by restrictive cellular factors that block viral replication in the cells of many species. In previous studies, we demonstrated that the restriction of CAEV infection of sheep choroid plexus cells was due to aberrant post-translation cleavage of the CAEV Env gp170 precursor. Later, we showed that the lack of specific receptor(s) for caprine encephalitis arthritis virus (CAEV) on the surface of human cells was the only barrier to their infection. Here, we examined whether small ruminant (SR) cells can support the replication of primate LVs. Three sheep and goat cell lines were inoculated with cell-free HIV-1 and SIVmac viral stocks or transfected with infectious molecular clone DNAs of these viruses. The two recombinant lentiviral clones contained the green fluorescent protein (GFP) reporter sequence. Infection was detected by GFP expression in target cells, and the infectious virus produced and released in the culture medium of treated cells was detected using the indicator TZM-bl cell line. Pseudotyped HIV-GFP and SIV-GFP with vesicular stomatitis virus G glycoprotein (VSV-G) allowed the cell receptors to be overcome for virus entry to further evaluate the viral replication/restriction in SR cells. As expected, neither HIV nor SIV viruses infected any of the SR cells. In contrast, the transfection of plasmid DNAs of the infectious molecular clones of both viruses in SR cells produced high titers of infectious viruses for human indicators, but not SR cell lines. Surprisingly, SR cells inoculated with HIV-GFP/VSV-G, but not SIV-GFP/VSV-G, expressed the GFP and produced a virus that efficiently infected the human indictor, but not the SR cells. Collectively, these data provide a demonstration of the lack of replication of the SIVmac genome in SR cells, while, in contrast, there was no restriction on the replication of the IV-1 genome in these cells. However, because of the lack of functional receptors to SIVmac and HIV-1 at the surface of SR cells, there is specific lentiviral entry.
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spelling pubmed-93164992022-07-27 Productive Replication of HIV-1 but Not SIVmac in Small Ruminant Cells Chergui, Hibet Errahmane Idres, Takfarinas Chaudesaigues, Chloé Noueihed, Diana Gagnon, Jean Chebloune, Yahia Pathogens Article Animal lentiviruses (LVs) have been proven to have the capacity to cross the species barrier, to adapt in the new hosts, and to increase their pathogenesis, therefore leading to the emergence of threatening diseases. However, their potential for widespread diffusion is limited by restrictive cellular factors that block viral replication in the cells of many species. In previous studies, we demonstrated that the restriction of CAEV infection of sheep choroid plexus cells was due to aberrant post-translation cleavage of the CAEV Env gp170 precursor. Later, we showed that the lack of specific receptor(s) for caprine encephalitis arthritis virus (CAEV) on the surface of human cells was the only barrier to their infection. Here, we examined whether small ruminant (SR) cells can support the replication of primate LVs. Three sheep and goat cell lines were inoculated with cell-free HIV-1 and SIVmac viral stocks or transfected with infectious molecular clone DNAs of these viruses. The two recombinant lentiviral clones contained the green fluorescent protein (GFP) reporter sequence. Infection was detected by GFP expression in target cells, and the infectious virus produced and released in the culture medium of treated cells was detected using the indicator TZM-bl cell line. Pseudotyped HIV-GFP and SIV-GFP with vesicular stomatitis virus G glycoprotein (VSV-G) allowed the cell receptors to be overcome for virus entry to further evaluate the viral replication/restriction in SR cells. As expected, neither HIV nor SIV viruses infected any of the SR cells. In contrast, the transfection of plasmid DNAs of the infectious molecular clones of both viruses in SR cells produced high titers of infectious viruses for human indicators, but not SR cell lines. Surprisingly, SR cells inoculated with HIV-GFP/VSV-G, but not SIV-GFP/VSV-G, expressed the GFP and produced a virus that efficiently infected the human indictor, but not the SR cells. Collectively, these data provide a demonstration of the lack of replication of the SIVmac genome in SR cells, while, in contrast, there was no restriction on the replication of the IV-1 genome in these cells. However, because of the lack of functional receptors to SIVmac and HIV-1 at the surface of SR cells, there is specific lentiviral entry. MDPI 2022-07-15 /pmc/articles/PMC9316499/ /pubmed/35890043 http://dx.doi.org/10.3390/pathogens11070799 Text en © 2022 by the authors. https://creativecommons.org/licenses/by/4.0/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 (https://creativecommons.org/licenses/by/4.0/).
spellingShingle Article
Chergui, Hibet Errahmane
Idres, Takfarinas
Chaudesaigues, Chloé
Noueihed, Diana
Gagnon, Jean
Chebloune, Yahia
Productive Replication of HIV-1 but Not SIVmac in Small Ruminant Cells
title Productive Replication of HIV-1 but Not SIVmac in Small Ruminant Cells
title_full Productive Replication of HIV-1 but Not SIVmac in Small Ruminant Cells
title_fullStr Productive Replication of HIV-1 but Not SIVmac in Small Ruminant Cells
title_full_unstemmed Productive Replication of HIV-1 but Not SIVmac in Small Ruminant Cells
title_short Productive Replication of HIV-1 but Not SIVmac in Small Ruminant Cells
title_sort productive replication of hiv-1 but not sivmac in small ruminant cells
topic Article
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC9316499/
https://www.ncbi.nlm.nih.gov/pubmed/35890043
http://dx.doi.org/10.3390/pathogens11070799
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