Evaluation of the innate immunostimulatory potential of originator and non-originator copies of insulin glargine in an in vitro human immune model

BACKGROUND: The manufacture of insulin analogs requires sophisticated production procedures which can lead to differences in the structure, purity, and/or other physiochemical properties of resultant products that can affect their biologic activity. Here, we sought to compare originator and non-orig...

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Autores principales: Luna, Ernesto, Agrawal, Pankaj, Mehta, Riyaz, Boone, Maria E., Vernhes, Charlotte, Denys, Colombe, Small, Robert, Mukherjee, Bhaswati, Tennagels, Norbert, Maerten, Stefan, Drake, Donald R.
Formato: Online Artículo Texto
Lenguaje:English
Publicado: Public Library of Science 2018
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Research Article
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC5991351/
https://www.ncbi.nlm.nih.gov/pubmed/29874257
http://dx.doi.org/10.1371/journal.pone.0197478
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author Luna, Ernesto
Agrawal, Pankaj
Mehta, Riyaz
Boone, Maria E.
Vernhes, Charlotte
Denys, Colombe
Small, Robert
Mukherjee, Bhaswati
Tennagels, Norbert
Maerten, Stefan
Drake, Donald R.
author_facet Luna, Ernesto
Agrawal, Pankaj
Mehta, Riyaz
Boone, Maria E.
Vernhes, Charlotte
Denys, Colombe
Small, Robert
Mukherjee, Bhaswati
Tennagels, Norbert
Maerten, Stefan
Drake, Donald R.
author_sort Luna, Ernesto
collection PubMed
description BACKGROUND: The manufacture of insulin analogs requires sophisticated production procedures which can lead to differences in the structure, purity, and/or other physiochemical properties of resultant products that can affect their biologic activity. Here, we sought to compare originator and non-originator copies of insulin glargine for innate immune activity and mechanisms leading to differences in these response profiles in an in vitro model of human immunity. METHODS: An endothelial/dendritic cell-based innate immune model was used to study antigen-presenting cell activation, cytokine secretion, and insulin receptor signalling pathways induced by originator and non-originator insulin glargine products. Mechanistic studies included signalling pathway blockade with specific inhibitors, analysis of the products in a Toll-like receptor reporter cell line assay, and natural insulin removal from the products by immunopurification. FINDINGS: All insulin glargine products elicited at least a minor innate immune response comparable to natural human insulin, but some lots of a non-originator copy product induced the elevated secretion of the cytokines, IL-8 and IL-6. In studies aimed at addressing the mechanisms leading to differential cytokine production by these products, we found (1) the inflammatory response was not mediated by bacterial contaminants, (2) the innate response was driven by the native insulin receptor through the MAPK pathway, and (3) the removal of insulin glargine significantly reduced their capacity to induce innate activity. No evidence of product aggregates was detected, though the presence of some high molecular weight proteins argues for the presence of insulin glargine dimers or others contaminants in these products. CONCLUSION: The data presented here suggests some non-originator insulin glargine product lots drive heightened in vitro human innate activity and provides preliminary evidence that changes in the biochemical composition of non-originator insulin glargine products (dimers, impurities) might be responsible for their greater immunostimulatory potential.
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spelling pubmed-59913512018-06-08 Evaluation of the innate immunostimulatory potential of originator and non-originator copies of insulin glargine in an in vitro human immune model Luna, Ernesto Agrawal, Pankaj Mehta, Riyaz Boone, Maria E. Vernhes, Charlotte Denys, Colombe Small, Robert Mukherjee, Bhaswati Tennagels, Norbert Maerten, Stefan Drake, Donald R. PLoS One Research Article BACKGROUND: The manufacture of insulin analogs requires sophisticated production procedures which can lead to differences in the structure, purity, and/or other physiochemical properties of resultant products that can affect their biologic activity. Here, we sought to compare originator and non-originator copies of insulin glargine for innate immune activity and mechanisms leading to differences in these response profiles in an in vitro model of human immunity. METHODS: An endothelial/dendritic cell-based innate immune model was used to study antigen-presenting cell activation, cytokine secretion, and insulin receptor signalling pathways induced by originator and non-originator insulin glargine products. Mechanistic studies included signalling pathway blockade with specific inhibitors, analysis of the products in a Toll-like receptor reporter cell line assay, and natural insulin removal from the products by immunopurification. FINDINGS: All insulin glargine products elicited at least a minor innate immune response comparable to natural human insulin, but some lots of a non-originator copy product induced the elevated secretion of the cytokines, IL-8 and IL-6. In studies aimed at addressing the mechanisms leading to differential cytokine production by these products, we found (1) the inflammatory response was not mediated by bacterial contaminants, (2) the innate response was driven by the native insulin receptor through the MAPK pathway, and (3) the removal of insulin glargine significantly reduced their capacity to induce innate activity. No evidence of product aggregates was detected, though the presence of some high molecular weight proteins argues for the presence of insulin glargine dimers or others contaminants in these products. CONCLUSION: The data presented here suggests some non-originator insulin glargine product lots drive heightened in vitro human innate activity and provides preliminary evidence that changes in the biochemical composition of non-originator insulin glargine products (dimers, impurities) might be responsible for their greater immunostimulatory potential. Public Library of Science 2018-06-06 /pmc/articles/PMC5991351/ /pubmed/29874257 http://dx.doi.org/10.1371/journal.pone.0197478 Text en © 2018 Luna et al http://creativecommons.org/licenses/by/4.0/ This is an open access article distributed under the terms of the Creative Commons Attribution License (http://creativecommons.org/licenses/by/4.0/) , which permits unrestricted use, distribution, and reproduction in any medium, provided the original author and source are credited.
spellingShingle Research Article
Luna, Ernesto
Agrawal, Pankaj
Mehta, Riyaz
Boone, Maria E.
Vernhes, Charlotte
Denys, Colombe
Small, Robert
Mukherjee, Bhaswati
Tennagels, Norbert
Maerten, Stefan
Drake, Donald R.
Evaluation of the innate immunostimulatory potential of originator and non-originator copies of insulin glargine in an in vitro human immune model
title Evaluation of the innate immunostimulatory potential of originator and non-originator copies of insulin glargine in an in vitro human immune model
title_full Evaluation of the innate immunostimulatory potential of originator and non-originator copies of insulin glargine in an in vitro human immune model
title_fullStr Evaluation of the innate immunostimulatory potential of originator and non-originator copies of insulin glargine in an in vitro human immune model
title_full_unstemmed Evaluation of the innate immunostimulatory potential of originator and non-originator copies of insulin glargine in an in vitro human immune model
title_short Evaluation of the innate immunostimulatory potential of originator and non-originator copies of insulin glargine in an in vitro human immune model
title_sort evaluation of the innate immunostimulatory potential of originator and non-originator copies of insulin glargine in an in vitro human immune model
topic Research Article
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC5991351/
https://www.ncbi.nlm.nih.gov/pubmed/29874257
http://dx.doi.org/10.1371/journal.pone.0197478
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