CCR5 Receptor Occupancy Analysis Reveals Increased Peripheral Blood CCR5+CD4+ T Cells Following Treatment With the Anti-CCR5 Antibody Leronlimab

CCR5 plays a central role in infectious disease, host defense, and cancer progression, thereby making it an ideal target for therapeutic development. Notably, CCR5 is the major HIV entry co-receptor, where its surface density correlates with HIV plasma viremia. The level of CCR5 receptor occupancy (...

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Autores principales: Chang, Xiao L., Wu, Helen L., Webb, Gabriela M., Tiwary, Meenakshi, Hughes, Colette, Reed, Jason S., Hwang, Joseph, Waytashek, Courtney, Boyle, Carla, Pessoa, Cleiton, Sylwester, Andrew W., Morrow, David, Belica, Karina, Fischer, Miranda, Kelly, Scott, Pourhassan, Nader, Bochart, Rachele M., Smedley, Jeremy, Recknor, Christopher P., Hansen, Scott G., Sacha, Jonah B.
Formato: Online Artículo Texto
Lenguaje:English
Publicado: Frontiers Media S.A. 2021
Materias:
Immunology
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC8640501/
https://www.ncbi.nlm.nih.gov/pubmed/34868084
http://dx.doi.org/10.3389/fimmu.2021.794638
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author Chang, Xiao L.
Wu, Helen L.
Webb, Gabriela M.
Tiwary, Meenakshi
Hughes, Colette
Reed, Jason S.
Hwang, Joseph
Waytashek, Courtney
Boyle, Carla
Pessoa, Cleiton
Sylwester, Andrew W.
Morrow, David
Belica, Karina
Fischer, Miranda
Kelly, Scott
Pourhassan, Nader
Bochart, Rachele M.
Smedley, Jeremy
Recknor, Christopher P.
Hansen, Scott G.
Sacha, Jonah B.
author_facet Chang, Xiao L.
Wu, Helen L.
Webb, Gabriela M.
Tiwary, Meenakshi
Hughes, Colette
Reed, Jason S.
Hwang, Joseph
Waytashek, Courtney
Boyle, Carla
Pessoa, Cleiton
Sylwester, Andrew W.
Morrow, David
Belica, Karina
Fischer, Miranda
Kelly, Scott
Pourhassan, Nader
Bochart, Rachele M.
Smedley, Jeremy
Recknor, Christopher P.
Hansen, Scott G.
Sacha, Jonah B.
author_sort Chang, Xiao L.
collection PubMed
description CCR5 plays a central role in infectious disease, host defense, and cancer progression, thereby making it an ideal target for therapeutic development. Notably, CCR5 is the major HIV entry co-receptor, where its surface density correlates with HIV plasma viremia. The level of CCR5 receptor occupancy (RO) achieved by a CCR5-targeting therapeutic is therefore a critical predictor of its efficacy. However, current methods to measure CCR5 RO lack sensitivity, resulting in high background and overcalculation. Here, we report on two independent, flow cytometric methods of calculating CCR5 RO using the anti-CCR5 antibody, Leronlimab. We show that both methods led to comparable CCR5 RO values, with low background on untreated CCR5+CD4+ T cells and sensitive measurements of occupancy on both blood and tissue-resident CD4+ T cells that correlated longitudinally with plasma concentrations in Leronlimab-treated macaques. Using these assays, we found that Leronlimab stabilized cell surface CCR5, leading to an increase in the levels of circulating and tissue-resident CCR5+CD4+ T cells in vivo in Leronlimab-treated macaques. Weekly Leronlimab treatment in a chronically SIV-infected macaque led to increased CCR5+CD4+ T cells levels and fully suppressed plasma viremia, both concomitant with full CCR5 RO on peripheral blood CD4+ T cells, demonstrating that CCR5+CD4+ T cells were protected from viral replication by Leronlimab binding. Finally, we extended these results to Leronlimab-treated humans and found that weekly 700 mg Leronlimab led to complete CCR5 RO on peripheral blood CD4+ T cells and a statistically significant increase in CCR5+CD4+ T cells in peripheral blood. Collectively, these results establish two RO calculation methods for longitudinal monitoring of anti-CCR5 therapeutic antibody blockade efficacy in both macaques and humans, demonstrate that CCR5+CD4+ T cell levels temporarily increase with Leronlimab treatment, and facilitate future detailed investigations into the immunological impacts of CCR5 inhibition in multiple pathophysiological processes.
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spelling pubmed-86405012021-12-04 CCR5 Receptor Occupancy Analysis Reveals Increased Peripheral Blood CCR5+CD4+ T Cells Following Treatment With the Anti-CCR5 Antibody Leronlimab Chang, Xiao L. Wu, Helen L. Webb, Gabriela M. Tiwary, Meenakshi Hughes, Colette Reed, Jason S. Hwang, Joseph Waytashek, Courtney Boyle, Carla Pessoa, Cleiton Sylwester, Andrew W. Morrow, David Belica, Karina Fischer, Miranda Kelly, Scott Pourhassan, Nader Bochart, Rachele M. Smedley, Jeremy Recknor, Christopher P. Hansen, Scott G. Sacha, Jonah B. Front Immunol Immunology CCR5 plays a central role in infectious disease, host defense, and cancer progression, thereby making it an ideal target for therapeutic development. Notably, CCR5 is the major HIV entry co-receptor, where its surface density correlates with HIV plasma viremia. The level of CCR5 receptor occupancy (RO) achieved by a CCR5-targeting therapeutic is therefore a critical predictor of its efficacy. However, current methods to measure CCR5 RO lack sensitivity, resulting in high background and overcalculation. Here, we report on two independent, flow cytometric methods of calculating CCR5 RO using the anti-CCR5 antibody, Leronlimab. We show that both methods led to comparable CCR5 RO values, with low background on untreated CCR5+CD4+ T cells and sensitive measurements of occupancy on both blood and tissue-resident CD4+ T cells that correlated longitudinally with plasma concentrations in Leronlimab-treated macaques. Using these assays, we found that Leronlimab stabilized cell surface CCR5, leading to an increase in the levels of circulating and tissue-resident CCR5+CD4+ T cells in vivo in Leronlimab-treated macaques. Weekly Leronlimab treatment in a chronically SIV-infected macaque led to increased CCR5+CD4+ T cells levels and fully suppressed plasma viremia, both concomitant with full CCR5 RO on peripheral blood CD4+ T cells, demonstrating that CCR5+CD4+ T cells were protected from viral replication by Leronlimab binding. Finally, we extended these results to Leronlimab-treated humans and found that weekly 700 mg Leronlimab led to complete CCR5 RO on peripheral blood CD4+ T cells and a statistically significant increase in CCR5+CD4+ T cells in peripheral blood. Collectively, these results establish two RO calculation methods for longitudinal monitoring of anti-CCR5 therapeutic antibody blockade efficacy in both macaques and humans, demonstrate that CCR5+CD4+ T cell levels temporarily increase with Leronlimab treatment, and facilitate future detailed investigations into the immunological impacts of CCR5 inhibition in multiple pathophysiological processes. Frontiers Media S.A. 2021-11-19 /pmc/articles/PMC8640501/ /pubmed/34868084 http://dx.doi.org/10.3389/fimmu.2021.794638 Text en Copyright © 2021 Chang, Wu, Webb, Tiwary, Hughes, Reed, Hwang, Waytashek, Boyle, Pessoa, Sylwester, Morrow, Belica, Fischer, Kelly, Pourhassan, Bochart, Smedley, Recknor, Hansen and Sacha https://creativecommons.org/licenses/by/4.0/This is an open-access article distributed under the terms of the Creative Commons Attribution License (CC BY). The use, distribution or reproduction in other forums is permitted, provided the original author(s) and the copyright owner(s) are credited and that the original publication in this journal is cited, in accordance with accepted academic practice. No use, distribution or reproduction is permitted which does not comply with these terms.
spellingShingle Immunology
Chang, Xiao L.
Wu, Helen L.
Webb, Gabriela M.
Tiwary, Meenakshi
Hughes, Colette
Reed, Jason S.
Hwang, Joseph
Waytashek, Courtney
Boyle, Carla
Pessoa, Cleiton
Sylwester, Andrew W.
Morrow, David
Belica, Karina
Fischer, Miranda
Kelly, Scott
Pourhassan, Nader
Bochart, Rachele M.
Smedley, Jeremy
Recknor, Christopher P.
Hansen, Scott G.
Sacha, Jonah B.
CCR5 Receptor Occupancy Analysis Reveals Increased Peripheral Blood CCR5+CD4+ T Cells Following Treatment With the Anti-CCR5 Antibody Leronlimab
title CCR5 Receptor Occupancy Analysis Reveals Increased Peripheral Blood CCR5+CD4+ T Cells Following Treatment With the Anti-CCR5 Antibody Leronlimab
title_full CCR5 Receptor Occupancy Analysis Reveals Increased Peripheral Blood CCR5+CD4+ T Cells Following Treatment With the Anti-CCR5 Antibody Leronlimab
title_fullStr CCR5 Receptor Occupancy Analysis Reveals Increased Peripheral Blood CCR5+CD4+ T Cells Following Treatment With the Anti-CCR5 Antibody Leronlimab
title_full_unstemmed CCR5 Receptor Occupancy Analysis Reveals Increased Peripheral Blood CCR5+CD4+ T Cells Following Treatment With the Anti-CCR5 Antibody Leronlimab
title_short CCR5 Receptor Occupancy Analysis Reveals Increased Peripheral Blood CCR5+CD4+ T Cells Following Treatment With the Anti-CCR5 Antibody Leronlimab
title_sort ccr5 receptor occupancy analysis reveals increased peripheral blood ccr5+cd4+ t cells following treatment with the anti-ccr5 antibody leronlimab
topic Immunology
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC8640501/
https://www.ncbi.nlm.nih.gov/pubmed/34868084
http://dx.doi.org/10.3389/fimmu.2021.794638
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