Development of new in vitro models of lung protease activity for investigating stability of inhaled biological therapies and drug delivery systems

Proteases play a vital role in lung health and are critically important to the metabolic clearance of inhaled protein-based therapeutics after inhalation. Surprisingly little is known about lung fluid protease composition and there is a consequent lack of biorelevant experimental models, which limit...

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Autores principales: Woods, Arcadia, Andrian, Teodora, Sharp, Gemma, Bicer, Elif Melis, Vandera, Kalliopi-Kelli A., Patel, Ayasha, Mudway, Ian, Dailey, Lea Ann, Forbes, Ben
Formato: Online Artículo Texto
Lenguaje:English
Publicado: Elsevier Science 2020
Materias:
Article
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC6963770/
https://www.ncbi.nlm.nih.gov/pubmed/31756380
http://dx.doi.org/10.1016/j.ejpb.2019.11.005
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author Woods, Arcadia
Andrian, Teodora
Sharp, Gemma
Bicer, Elif Melis
Vandera, Kalliopi-Kelli A.
Patel, Ayasha
Mudway, Ian
Dailey, Lea Ann
Forbes, Ben
author_facet Woods, Arcadia
Andrian, Teodora
Sharp, Gemma
Bicer, Elif Melis
Vandera, Kalliopi-Kelli A.
Patel, Ayasha
Mudway, Ian
Dailey, Lea Ann
Forbes, Ben
author_sort Woods, Arcadia
collection PubMed
description Proteases play a vital role in lung health and are critically important to the metabolic clearance of inhaled protein-based therapeutics after inhalation. Surprisingly little is known about lung fluid protease composition and there is a consequent lack of biorelevant experimental models, which limits research and development in the burgeoning field of inhaled biologics. The aim of this study was to quantify proteases in human lung fluid and to use this data to design novel in vitro experimental models of lung lining fluid possessing biorelevant lung protease activity for use in biopharmaceutical stability studies. As a proof of concept, these novel models were used to investigate the effect of proteolytic activity on the stability of albumin nanoparticles, a biologic nanoparticle formulation widely investigated as a pulmonary drug delivery system. Bronchoalveolar lavage fluid was collected from healthy human volunteers and proteomic analysis was used to quantify the predominant proteases. Based on these data, four new lung protease models were constructed based on: (i) trypsin as a sole protease, (ii) dipeptidyl peptidase IV, cathepsin D, cathepsin H, and angiotensin converting enzyme in ratio and concentration to mimic the protease concentration in healthy lungs. Neutrophil elastase was used to model protease activity in inflammation. Albumin nanoparticles of 100 nm diameter remained intact over 48 h in phosphate buffered saline, but were degraded more rapidly in trypsin (50% reduction in 10 min) compared to the healthy lung protease model (50% reduction in 150 min). The addition of neutrophil elastase to the healthy lung protease model resulted in a similar, but more variable degradation profile. Nanoparticle degradation was associated with concomitant appearance of small fragments and aggregates. In conclusion, we have characterised the protease concentration in the lungs of healthy humans, designed models of lung protease activity and demonstrated their utility in studying albumin nanoparticle degradation. These methods and models have wide application to study the influence of proteases in lung disease, expression of proteases in respiratory cell culture models, stability of peptide and protein-based drugs and inhaled drug delivery systems.
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spelling pubmed-69637702020-01-22 Development of new in vitro models of lung protease activity for investigating stability of inhaled biological therapies and drug delivery systems Woods, Arcadia Andrian, Teodora Sharp, Gemma Bicer, Elif Melis Vandera, Kalliopi-Kelli A. Patel, Ayasha Mudway, Ian Dailey, Lea Ann Forbes, Ben Eur J Pharm Biopharm Article Proteases play a vital role in lung health and are critically important to the metabolic clearance of inhaled protein-based therapeutics after inhalation. Surprisingly little is known about lung fluid protease composition and there is a consequent lack of biorelevant experimental models, which limits research and development in the burgeoning field of inhaled biologics. The aim of this study was to quantify proteases in human lung fluid and to use this data to design novel in vitro experimental models of lung lining fluid possessing biorelevant lung protease activity for use in biopharmaceutical stability studies. As a proof of concept, these novel models were used to investigate the effect of proteolytic activity on the stability of albumin nanoparticles, a biologic nanoparticle formulation widely investigated as a pulmonary drug delivery system. Bronchoalveolar lavage fluid was collected from healthy human volunteers and proteomic analysis was used to quantify the predominant proteases. Based on these data, four new lung protease models were constructed based on: (i) trypsin as a sole protease, (ii) dipeptidyl peptidase IV, cathepsin D, cathepsin H, and angiotensin converting enzyme in ratio and concentration to mimic the protease concentration in healthy lungs. Neutrophil elastase was used to model protease activity in inflammation. Albumin nanoparticles of 100 nm diameter remained intact over 48 h in phosphate buffered saline, but were degraded more rapidly in trypsin (50% reduction in 10 min) compared to the healthy lung protease model (50% reduction in 150 min). The addition of neutrophil elastase to the healthy lung protease model resulted in a similar, but more variable degradation profile. Nanoparticle degradation was associated with concomitant appearance of small fragments and aggregates. In conclusion, we have characterised the protease concentration in the lungs of healthy humans, designed models of lung protease activity and demonstrated their utility in studying albumin nanoparticle degradation. These methods and models have wide application to study the influence of proteases in lung disease, expression of proteases in respiratory cell culture models, stability of peptide and protein-based drugs and inhaled drug delivery systems. Elsevier Science 2020-01 /pmc/articles/PMC6963770/ /pubmed/31756380 http://dx.doi.org/10.1016/j.ejpb.2019.11.005 Text en © 2019 The Author(s) http://creativecommons.org/licenses/by/4.0/ This is an open access article under the CC BY license (http://creativecommons.org/licenses/by/4.0/).
spellingShingle Article
Woods, Arcadia
Andrian, Teodora
Sharp, Gemma
Bicer, Elif Melis
Vandera, Kalliopi-Kelli A.
Patel, Ayasha
Mudway, Ian
Dailey, Lea Ann
Forbes, Ben
Development of new in vitro models of lung protease activity for investigating stability of inhaled biological therapies and drug delivery systems
title Development of new in vitro models of lung protease activity for investigating stability of inhaled biological therapies and drug delivery systems
title_full Development of new in vitro models of lung protease activity for investigating stability of inhaled biological therapies and drug delivery systems
title_fullStr Development of new in vitro models of lung protease activity for investigating stability of inhaled biological therapies and drug delivery systems
title_full_unstemmed Development of new in vitro models of lung protease activity for investigating stability of inhaled biological therapies and drug delivery systems
title_short Development of new in vitro models of lung protease activity for investigating stability of inhaled biological therapies and drug delivery systems
title_sort development of new in vitro models of lung protease activity for investigating stability of inhaled biological therapies and drug delivery systems
topic Article
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC6963770/
https://www.ncbi.nlm.nih.gov/pubmed/31756380
http://dx.doi.org/10.1016/j.ejpb.2019.11.005
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