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HIV-1 envelope, integrins and co-receptor use in mucosal transmission of HIV

It is well established that HIV-1 infection typically involves an interaction between the viral envelope protein gp120/41 and the CD4 molecule followed by a second interaction with a chemokine receptor, usually CCR5 or CXCR4. In the early stages of an HIV-1 infection CCR5 using viruses (R5 viruses)...

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Autores principales: Cicala, Claudia, Arthos, James, Fauci, Anthony S
Formato: Texto
Lenguaje:English
Publicado: BioMed Central 2011
Materias:
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC3105502/
https://www.ncbi.nlm.nih.gov/pubmed/21284901
http://dx.doi.org/10.1186/1479-5876-9-S1-S2
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author Cicala, Claudia
Arthos, James
Fauci, Anthony S
author_facet Cicala, Claudia
Arthos, James
Fauci, Anthony S
author_sort Cicala, Claudia
collection PubMed
description It is well established that HIV-1 infection typically involves an interaction between the viral envelope protein gp120/41 and the CD4 molecule followed by a second interaction with a chemokine receptor, usually CCR5 or CXCR4. In the early stages of an HIV-1 infection CCR5 using viruses (R5 viruses) predominate. In some viral subtypes there is a propensity to switch to CXCR4 usage (X4 viruses). The receptor switch occurs in ~ 40% of the infected individuals and is associated with faster disease progression. This holds for subtypes B and D, but occurs less frequently in subtypes A and C. There are several hypotheses to explain the preferential transmission of R5 viruses and the mechanisms that lead to switching of co-receptor usage; however, there is no definitive explanation for either. One important consideration regarding transmission is that signaling by R5 gp120 may facilitate transmission of R5 viruses by inducing a permissive environment for HIV replication. In the case of sexual transmission, infection by HIV requires the virus to breach the mucosal barrier to gain access to the immune cell targets that it infects; however, the immediate events that follow HIV exposure at genital mucosal sites are not well understood. Upon transmission, the HIV quasispecies that is replicating in an infected donor contracts through a “genetic bottleneck”, and often infection results from a single infectious event. Many details surrounding this initial infection remain unresolved. In mucosal tissues, CD4(+) T cells express high levels of CCR5, and a subset of these CD4(+)/CCR5(high) cells express the integrin α(4)β(7), the gut homing receptor. CD4(+)/CCR5(high)/ α4β7(high) T cells are highly susceptible to infection by HIV-1 and are ideal targets for an efficient productive infection at the point of transmission. In this context we have demonstrated that the HIV-1 envelope protein gp120 binds to α(4)β(7) on CD4(+) T cells. On CD4(+)/CCR5(high)/ α4β7(high) T cells, α(4)β(7) is closely associated with CD4 and CCR5. Furthermore, α(4)β(7) is ~3 times the size of CD4 on the cell surface, that makes it a prominent receptor for an efficient virus capture. gp120-α(4)β(7) interactions mediate the activation of the adhesion-associated integrin LFA-1. LFA-1 facilitates the formation of virological synapses and cell-to-cell spread of HIV-1. gp120 binding to α(4)β(7) is mediated by a tripeptide located in the V1/V2 domain of gp120. Of note, the V1/V2 domain of gp120 has been linked to variations in transmission fitness among viral isolates raising the intriguing possibility that gp120-α(4)β(7) interactions may be linked to transmission fitness. Although many details remain unresolved, we hypothesize that gp120-α(4)β(7) interactions play an important role in the very early events following sexual transmission of HIV and may have important implication in the design of vaccine strategies for the prevention of acquisition of HIV infection
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spelling pubmed-31055022011-06-02 HIV-1 envelope, integrins and co-receptor use in mucosal transmission of HIV Cicala, Claudia Arthos, James Fauci, Anthony S J Transl Med Review It is well established that HIV-1 infection typically involves an interaction between the viral envelope protein gp120/41 and the CD4 molecule followed by a second interaction with a chemokine receptor, usually CCR5 or CXCR4. In the early stages of an HIV-1 infection CCR5 using viruses (R5 viruses) predominate. In some viral subtypes there is a propensity to switch to CXCR4 usage (X4 viruses). The receptor switch occurs in ~ 40% of the infected individuals and is associated with faster disease progression. This holds for subtypes B and D, but occurs less frequently in subtypes A and C. There are several hypotheses to explain the preferential transmission of R5 viruses and the mechanisms that lead to switching of co-receptor usage; however, there is no definitive explanation for either. One important consideration regarding transmission is that signaling by R5 gp120 may facilitate transmission of R5 viruses by inducing a permissive environment for HIV replication. In the case of sexual transmission, infection by HIV requires the virus to breach the mucosal barrier to gain access to the immune cell targets that it infects; however, the immediate events that follow HIV exposure at genital mucosal sites are not well understood. Upon transmission, the HIV quasispecies that is replicating in an infected donor contracts through a “genetic bottleneck”, and often infection results from a single infectious event. Many details surrounding this initial infection remain unresolved. In mucosal tissues, CD4(+) T cells express high levels of CCR5, and a subset of these CD4(+)/CCR5(high) cells express the integrin α(4)β(7), the gut homing receptor. CD4(+)/CCR5(high)/ α4β7(high) T cells are highly susceptible to infection by HIV-1 and are ideal targets for an efficient productive infection at the point of transmission. In this context we have demonstrated that the HIV-1 envelope protein gp120 binds to α(4)β(7) on CD4(+) T cells. On CD4(+)/CCR5(high)/ α4β7(high) T cells, α(4)β(7) is closely associated with CD4 and CCR5. Furthermore, α(4)β(7) is ~3 times the size of CD4 on the cell surface, that makes it a prominent receptor for an efficient virus capture. gp120-α(4)β(7) interactions mediate the activation of the adhesion-associated integrin LFA-1. LFA-1 facilitates the formation of virological synapses and cell-to-cell spread of HIV-1. gp120 binding to α(4)β(7) is mediated by a tripeptide located in the V1/V2 domain of gp120. Of note, the V1/V2 domain of gp120 has been linked to variations in transmission fitness among viral isolates raising the intriguing possibility that gp120-α(4)β(7) interactions may be linked to transmission fitness. Although many details remain unresolved, we hypothesize that gp120-α(4)β(7) interactions play an important role in the very early events following sexual transmission of HIV and may have important implication in the design of vaccine strategies for the prevention of acquisition of HIV infection BioMed Central 2011-01-27 /pmc/articles/PMC3105502/ /pubmed/21284901 http://dx.doi.org/10.1186/1479-5876-9-S1-S2 Text en Copyright ©2011 Cicala et al; licensee BioMed Central Ltd. This is an open access article distributed under the terms of the Creative Commons Attribution License (<url>http://creativecommons.org/licenses/by/2.0</url>), which permits unrestricted use, distribution, and reproduction in any medium, provided the original work is properly cited.
spellingShingle Review
Cicala, Claudia
Arthos, James
Fauci, Anthony S
HIV-1 envelope, integrins and co-receptor use in mucosal transmission of HIV
title HIV-1 envelope, integrins and co-receptor use in mucosal transmission of HIV
title_full HIV-1 envelope, integrins and co-receptor use in mucosal transmission of HIV
title_fullStr HIV-1 envelope, integrins and co-receptor use in mucosal transmission of HIV
title_full_unstemmed HIV-1 envelope, integrins and co-receptor use in mucosal transmission of HIV
title_short HIV-1 envelope, integrins and co-receptor use in mucosal transmission of HIV
title_sort hiv-1 envelope, integrins and co-receptor use in mucosal transmission of hiv
topic Review
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC3105502/
https://www.ncbi.nlm.nih.gov/pubmed/21284901
http://dx.doi.org/10.1186/1479-5876-9-S1-S2
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