Evaluation of IL-1 Blockade as an Adjunct to Linezolid Therapy for Tuberculosis in Mice and Macaques

In 2017 over 550,000 estimated new cases of multi-drug/rifampicin resistant tuberculosis (MDR/RR-TB) occurred, emphasizing a need for new treatment strategies. Linezolid (LZD) is a potent antibiotic for drug-resistant Gram-positive infections and is an effective treatment for TB. However, extended L...

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Autores principales: Winchell, Caylin G., Mishra, Bibhuti B., Phuah, Jia Yao, Saqib, Mohd, Nelson, Samantha J., Maiello, Pauline, Causgrove, Chelsea M., Ameel, Cassaundra L., Stein, Brianne, Borish, H. Jacob, White, Alexander G., Klein, Edwin C., Zimmerman, Matthew D., Dartois, Véronique, Lin, Philana Ling, Sassetti, Christopher M., Flynn, JoAnne L.
Formato: Online Artículo Texto
Lenguaje:English
Publicado: Frontiers Media S.A. 2020
Materias:
Immunology
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC7235418/
https://www.ncbi.nlm.nih.gov/pubmed/32477361
http://dx.doi.org/10.3389/fimmu.2020.00891
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author Winchell, Caylin G.
Mishra, Bibhuti B.
Phuah, Jia Yao
Saqib, Mohd
Nelson, Samantha J.
Maiello, Pauline
Causgrove, Chelsea M.
Ameel, Cassaundra L.
Stein, Brianne
Borish, H. Jacob
White, Alexander G.
Klein, Edwin C.
Zimmerman, Matthew D.
Dartois, Véronique
Lin, Philana Ling
Sassetti, Christopher M.
Flynn, JoAnne L.
author_facet Winchell, Caylin G.
Mishra, Bibhuti B.
Phuah, Jia Yao
Saqib, Mohd
Nelson, Samantha J.
Maiello, Pauline
Causgrove, Chelsea M.
Ameel, Cassaundra L.
Stein, Brianne
Borish, H. Jacob
White, Alexander G.
Klein, Edwin C.
Zimmerman, Matthew D.
Dartois, Véronique
Lin, Philana Ling
Sassetti, Christopher M.
Flynn, JoAnne L.
author_sort Winchell, Caylin G.
collection PubMed
description In 2017 over 550,000 estimated new cases of multi-drug/rifampicin resistant tuberculosis (MDR/RR-TB) occurred, emphasizing a need for new treatment strategies. Linezolid (LZD) is a potent antibiotic for drug-resistant Gram-positive infections and is an effective treatment for TB. However, extended LZD use can lead to LZD-associated host toxicities, most commonly bone marrow suppression. LZD toxicities may be mediated by IL-1, an inflammatory pathway important for early immunity during M. tuberculosis infection. However, IL-1 can contribute to pathology and disease severity late in TB progression. Since IL-1 may contribute to LZD toxicity and does influence TB pathology, we targeted this pathway with a potential host-directed therapy (HDT). We hypothesized LZD efficacy could be enhanced by modulation of IL-1 pathway to reduce bone marrow toxicity and TB associated-inflammation. We used two animal models of TB to test our hypothesis, a TB-susceptible mouse model and clinically relevant cynomolgus macaques. Antagonizing IL-1 in mice with established infection reduced lung neutrophil numbers and partially restored the erythroid progenitor populations that are depleted by LZD. In macaques, we found no conclusive evidence of bone marrow suppression associated with LZD, indicating our treatment time may have been short enough to avoid the toxicities observed in humans. Though treatment was only 4 weeks (the FDA approved regimen at the time of study), we observed sterilization of the majority of granulomas regardless of co-administration of the FDA-approved IL-1 receptor antagonist (IL-1Rn), also known as Anakinra. However, total lung inflammation was significantly reduced in macaques treated with IL-1Rn and LZD compared to LZD alone. Importantly, IL-1Rn administration did not impair the host response against Mtb or LZD efficacy in either animal model. Together, our data support that inhibition of IL-1 in combination with LZD has potential to be an effective HDT for TB and the need for further research in this area.
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spelling pubmed-72354182020-05-29 Evaluation of IL-1 Blockade as an Adjunct to Linezolid Therapy for Tuberculosis in Mice and Macaques Winchell, Caylin G. Mishra, Bibhuti B. Phuah, Jia Yao Saqib, Mohd Nelson, Samantha J. Maiello, Pauline Causgrove, Chelsea M. Ameel, Cassaundra L. Stein, Brianne Borish, H. Jacob White, Alexander G. Klein, Edwin C. Zimmerman, Matthew D. Dartois, Véronique Lin, Philana Ling Sassetti, Christopher M. Flynn, JoAnne L. Front Immunol Immunology In 2017 over 550,000 estimated new cases of multi-drug/rifampicin resistant tuberculosis (MDR/RR-TB) occurred, emphasizing a need for new treatment strategies. Linezolid (LZD) is a potent antibiotic for drug-resistant Gram-positive infections and is an effective treatment for TB. However, extended LZD use can lead to LZD-associated host toxicities, most commonly bone marrow suppression. LZD toxicities may be mediated by IL-1, an inflammatory pathway important for early immunity during M. tuberculosis infection. However, IL-1 can contribute to pathology and disease severity late in TB progression. Since IL-1 may contribute to LZD toxicity and does influence TB pathology, we targeted this pathway with a potential host-directed therapy (HDT). We hypothesized LZD efficacy could be enhanced by modulation of IL-1 pathway to reduce bone marrow toxicity and TB associated-inflammation. We used two animal models of TB to test our hypothesis, a TB-susceptible mouse model and clinically relevant cynomolgus macaques. Antagonizing IL-1 in mice with established infection reduced lung neutrophil numbers and partially restored the erythroid progenitor populations that are depleted by LZD. In macaques, we found no conclusive evidence of bone marrow suppression associated with LZD, indicating our treatment time may have been short enough to avoid the toxicities observed in humans. Though treatment was only 4 weeks (the FDA approved regimen at the time of study), we observed sterilization of the majority of granulomas regardless of co-administration of the FDA-approved IL-1 receptor antagonist (IL-1Rn), also known as Anakinra. However, total lung inflammation was significantly reduced in macaques treated with IL-1Rn and LZD compared to LZD alone. Importantly, IL-1Rn administration did not impair the host response against Mtb or LZD efficacy in either animal model. Together, our data support that inhibition of IL-1 in combination with LZD has potential to be an effective HDT for TB and the need for further research in this area. Frontiers Media S.A. 2020-05-12 /pmc/articles/PMC7235418/ /pubmed/32477361 http://dx.doi.org/10.3389/fimmu.2020.00891 Text en Copyright © 2020 Winchell, Mishra, Phuah, Saqib, Nelson, Maiello, Causgrove, Ameel, Stein, Borish, White, Klein, Zimmerman, Dartois, Lin, Sassetti and Flynn. http://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
Winchell, Caylin G.
Mishra, Bibhuti B.
Phuah, Jia Yao
Saqib, Mohd
Nelson, Samantha J.
Maiello, Pauline
Causgrove, Chelsea M.
Ameel, Cassaundra L.
Stein, Brianne
Borish, H. Jacob
White, Alexander G.
Klein, Edwin C.
Zimmerman, Matthew D.
Dartois, Véronique
Lin, Philana Ling
Sassetti, Christopher M.
Flynn, JoAnne L.
Evaluation of IL-1 Blockade as an Adjunct to Linezolid Therapy for Tuberculosis in Mice and Macaques
title Evaluation of IL-1 Blockade as an Adjunct to Linezolid Therapy for Tuberculosis in Mice and Macaques
title_full Evaluation of IL-1 Blockade as an Adjunct to Linezolid Therapy for Tuberculosis in Mice and Macaques
title_fullStr Evaluation of IL-1 Blockade as an Adjunct to Linezolid Therapy for Tuberculosis in Mice and Macaques
title_full_unstemmed Evaluation of IL-1 Blockade as an Adjunct to Linezolid Therapy for Tuberculosis in Mice and Macaques
title_short Evaluation of IL-1 Blockade as an Adjunct to Linezolid Therapy for Tuberculosis in Mice and Macaques
title_sort evaluation of il-1 blockade as an adjunct to linezolid therapy for tuberculosis in mice and macaques
topic Immunology
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC7235418/
https://www.ncbi.nlm.nih.gov/pubmed/32477361
http://dx.doi.org/10.3389/fimmu.2020.00891
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