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MAdCAM costimulation through Integrin-α(4)β(7) promotes HIV replication

Human gut associated lymphoid tissues (GALT) play a key role in the acute phase of HIV infection. The propensity of HIV to replicate in these tissues however, is not fully understood. Access and migration of naïve and memory CD4(+) T cells to these sites is mediated by interactions between integrin...

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Autores principales: Nawaz, Fatima, Goes, Livia R., Ray, Jocelyn C., Olowojesiku, Ronke, Sajani, Alia, Ansari, Aftab A., Perrone, Ian, Hiatt, Joseph, Van Ryk, Donald, Wei, Danlan, Waliszewski, Mia, Soares, Marcelo A., Jelicic, Katija, Connors, Mark, Migueles, Stephen A., Martinelli, Elena, Villinger, Francois, Cicala, Claudia, Fauci, Anthony S., Arthos, James
Formato: Online Artículo Texto
Lenguaje:English
Publicado: 2018
Materias:
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC6160318/
https://www.ncbi.nlm.nih.gov/pubmed/29875402
http://dx.doi.org/10.1038/s41385-018-0044-1
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author Nawaz, Fatima
Goes, Livia R.
Ray, Jocelyn C.
Olowojesiku, Ronke
Sajani, Alia
Ansari, Aftab A.
Perrone, Ian
Hiatt, Joseph
Van Ryk, Donald
Wei, Danlan
Waliszewski, Mia
Soares, Marcelo A.
Jelicic, Katija
Connors, Mark
Migueles, Stephen A.
Martinelli, Elena
Villinger, Francois
Cicala, Claudia
Fauci, Anthony S.
Arthos, James
author_facet Nawaz, Fatima
Goes, Livia R.
Ray, Jocelyn C.
Olowojesiku, Ronke
Sajani, Alia
Ansari, Aftab A.
Perrone, Ian
Hiatt, Joseph
Van Ryk, Donald
Wei, Danlan
Waliszewski, Mia
Soares, Marcelo A.
Jelicic, Katija
Connors, Mark
Migueles, Stephen A.
Martinelli, Elena
Villinger, Francois
Cicala, Claudia
Fauci, Anthony S.
Arthos, James
author_sort Nawaz, Fatima
collection PubMed
description Human gut associated lymphoid tissues (GALT) play a key role in the acute phase of HIV infection. The propensity of HIV to replicate in these tissues however, is not fully understood. Access and migration of naïve and memory CD4(+) T cells to these sites is mediated by interactions between integrin α(4)β(7), expressed on CD4(+) T cells, and MAdCAM, expressed on high endothelial venules. We report here that MAdCAM delivers a potent costimulatory signal to naïve and memory CD4(+) T cells following ligation with α(4)β(7). Such costimulation promotes high-levels of HIV replication. An anti-α(4)β(7) mAb that prevents mucosal transmission of SIV blocks MAdCAM signaling through α(4)β(7) and MAdCAM-dependent viral replication. MAdCAM costimulation of memory CD4(+) T cells is sufficient to drive cellular proliferation and the up-regulation of CCR5, while naïve CD4(+) T cells require both MAdCAM and retinoic acid to achieve the same response. The pairing of MAdCAM and retinoic acid is unique to the GALT, leading us to propose that HIV replication in these sites is facilitated by MAdCAM-α(4)β(7) interactions. Moreover, complete inhibition of MAdCAM signaling by an anti-α(4)β(7) mAb, an analogue of a clinically approved therapeutic (vedolizumab), highlights the potential of such agents to control acute HIV infection.
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spelling pubmed-61603182018-12-06 MAdCAM costimulation through Integrin-α(4)β(7) promotes HIV replication Nawaz, Fatima Goes, Livia R. Ray, Jocelyn C. Olowojesiku, Ronke Sajani, Alia Ansari, Aftab A. Perrone, Ian Hiatt, Joseph Van Ryk, Donald Wei, Danlan Waliszewski, Mia Soares, Marcelo A. Jelicic, Katija Connors, Mark Migueles, Stephen A. Martinelli, Elena Villinger, Francois Cicala, Claudia Fauci, Anthony S. Arthos, James Mucosal Immunol Article Human gut associated lymphoid tissues (GALT) play a key role in the acute phase of HIV infection. The propensity of HIV to replicate in these tissues however, is not fully understood. Access and migration of naïve and memory CD4(+) T cells to these sites is mediated by interactions between integrin α(4)β(7), expressed on CD4(+) T cells, and MAdCAM, expressed on high endothelial venules. We report here that MAdCAM delivers a potent costimulatory signal to naïve and memory CD4(+) T cells following ligation with α(4)β(7). Such costimulation promotes high-levels of HIV replication. An anti-α(4)β(7) mAb that prevents mucosal transmission of SIV blocks MAdCAM signaling through α(4)β(7) and MAdCAM-dependent viral replication. MAdCAM costimulation of memory CD4(+) T cells is sufficient to drive cellular proliferation and the up-regulation of CCR5, while naïve CD4(+) T cells require both MAdCAM and retinoic acid to achieve the same response. The pairing of MAdCAM and retinoic acid is unique to the GALT, leading us to propose that HIV replication in these sites is facilitated by MAdCAM-α(4)β(7) interactions. Moreover, complete inhibition of MAdCAM signaling by an anti-α(4)β(7) mAb, an analogue of a clinically approved therapeutic (vedolizumab), highlights the potential of such agents to control acute HIV infection. 2018-06-06 2018-09 /pmc/articles/PMC6160318/ /pubmed/29875402 http://dx.doi.org/10.1038/s41385-018-0044-1 Text en http://www.nature.com/authors/editorial_policies/license.html#terms Users may view, print, copy, and download text and data-mine the content in such documents, for the purposes of academic research, subject always to the full Conditions of use:http://www.nature.com/authors/editorial_policies/license.html#terms
spellingShingle Article
Nawaz, Fatima
Goes, Livia R.
Ray, Jocelyn C.
Olowojesiku, Ronke
Sajani, Alia
Ansari, Aftab A.
Perrone, Ian
Hiatt, Joseph
Van Ryk, Donald
Wei, Danlan
Waliszewski, Mia
Soares, Marcelo A.
Jelicic, Katija
Connors, Mark
Migueles, Stephen A.
Martinelli, Elena
Villinger, Francois
Cicala, Claudia
Fauci, Anthony S.
Arthos, James
MAdCAM costimulation through Integrin-α(4)β(7) promotes HIV replication
title MAdCAM costimulation through Integrin-α(4)β(7) promotes HIV replication
title_full MAdCAM costimulation through Integrin-α(4)β(7) promotes HIV replication
title_fullStr MAdCAM costimulation through Integrin-α(4)β(7) promotes HIV replication
title_full_unstemmed MAdCAM costimulation through Integrin-α(4)β(7) promotes HIV replication
title_short MAdCAM costimulation through Integrin-α(4)β(7) promotes HIV replication
title_sort madcam costimulation through integrin-α(4)β(7) promotes hiv replication
topic Article
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC6160318/
https://www.ncbi.nlm.nih.gov/pubmed/29875402
http://dx.doi.org/10.1038/s41385-018-0044-1
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