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Rapid Developability Assessments to Formulate Recombinant Protein Antigens as Stable, Low-Cost, Multi-Dose Vaccine Candidates: Case-Study With Non-Replicating Rotavirus (NRRV) Vaccine Antigens

A two-step developability assessment workflow is described to screen variants of recombinant protein antigens under various formulation conditions to rapidly identify stable, aluminum-adjuvanted, multi-dose vaccine candidates. For proof-of-concept, a series of sequence variants of the recombinant no...

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Autores principales: Sawant, Nishant, Kaur, Kawaljit, Holland, David A., Hickey, John M., Agarwal, Sanjeev, Brady, Joseph R., Dalvie, Neil C., Tracey, Mary Kate, Velez-Suberbie, M. Lourdes, Morris, Stephen A., Jacob, Shaleem I., Bracewell, Daniel G., Mukhopadhyay, Tarit K., Love, Kerry R., Love, J. Christopher, Joshi, Sangeeta B., Volkin, David B.
Formato: Online Artículo Texto
Lenguaje:English
Publicado: Elsevier 2021
Materias:
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC7884052/
https://www.ncbi.nlm.nih.gov/pubmed/33285182
http://dx.doi.org/10.1016/j.xphs.2020.11.039
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author Sawant, Nishant
Kaur, Kawaljit
Holland, David A.
Hickey, John M.
Agarwal, Sanjeev
Brady, Joseph R.
Dalvie, Neil C.
Tracey, Mary Kate
Velez-Suberbie, M. Lourdes
Morris, Stephen A.
Jacob, Shaleem I.
Bracewell, Daniel G.
Mukhopadhyay, Tarit K.
Love, Kerry R.
Love, J. Christopher
Joshi, Sangeeta B.
Volkin, David B.
author_facet Sawant, Nishant
Kaur, Kawaljit
Holland, David A.
Hickey, John M.
Agarwal, Sanjeev
Brady, Joseph R.
Dalvie, Neil C.
Tracey, Mary Kate
Velez-Suberbie, M. Lourdes
Morris, Stephen A.
Jacob, Shaleem I.
Bracewell, Daniel G.
Mukhopadhyay, Tarit K.
Love, Kerry R.
Love, J. Christopher
Joshi, Sangeeta B.
Volkin, David B.
author_sort Sawant, Nishant
collection PubMed
description A two-step developability assessment workflow is described to screen variants of recombinant protein antigens under various formulation conditions to rapidly identify stable, aluminum-adjuvanted, multi-dose vaccine candidates. For proof-of-concept, a series of sequence variants of the recombinant non-replicating rotavirus (NRRV) P[8] protein antigen (produced in Komagataella phaffii) were compared in terms of primary structure, post-translational modifications, antibody binding, conformational stability, relative solubility and preservative compatibility. Based on these results, promising P[8] variants were down-selected and the impact of key formulation conditions on storage stability was examined (e.g., presence or absence of the aluminum-adjuvant Alhydrogel and the preservative thimerosal) as measured by differential scanning calorimetry (DSC) and antibody binding assays. Good correlations between rapidly-generated developability screening data and storage stability profiles (12 weeks at various temperatures) were observed for aluminum-adsorbed P[8] antigens. These findings were extended and confirmed using variants of a second NRRV antigen, P[4]. These case-study results with P[8] and P[4] NRRV variants are discussed in terms of using this vaccine formulation developability workflow to better inform and optimize formulation design with a wide variety of recombinant protein antigens, with the long-term goal of rapidly and cost-efficiently identifying low-cost vaccine formulations for use in low and middle income countries.
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spelling pubmed-78840522021-03-01 Rapid Developability Assessments to Formulate Recombinant Protein Antigens as Stable, Low-Cost, Multi-Dose Vaccine Candidates: Case-Study With Non-Replicating Rotavirus (NRRV) Vaccine Antigens Sawant, Nishant Kaur, Kawaljit Holland, David A. Hickey, John M. Agarwal, Sanjeev Brady, Joseph R. Dalvie, Neil C. Tracey, Mary Kate Velez-Suberbie, M. Lourdes Morris, Stephen A. Jacob, Shaleem I. Bracewell, Daniel G. Mukhopadhyay, Tarit K. Love, Kerry R. Love, J. Christopher Joshi, Sangeeta B. Volkin, David B. J Pharm Sci Research Article A two-step developability assessment workflow is described to screen variants of recombinant protein antigens under various formulation conditions to rapidly identify stable, aluminum-adjuvanted, multi-dose vaccine candidates. For proof-of-concept, a series of sequence variants of the recombinant non-replicating rotavirus (NRRV) P[8] protein antigen (produced in Komagataella phaffii) were compared in terms of primary structure, post-translational modifications, antibody binding, conformational stability, relative solubility and preservative compatibility. Based on these results, promising P[8] variants were down-selected and the impact of key formulation conditions on storage stability was examined (e.g., presence or absence of the aluminum-adjuvant Alhydrogel and the preservative thimerosal) as measured by differential scanning calorimetry (DSC) and antibody binding assays. Good correlations between rapidly-generated developability screening data and storage stability profiles (12 weeks at various temperatures) were observed for aluminum-adsorbed P[8] antigens. These findings were extended and confirmed using variants of a second NRRV antigen, P[4]. These case-study results with P[8] and P[4] NRRV variants are discussed in terms of using this vaccine formulation developability workflow to better inform and optimize formulation design with a wide variety of recombinant protein antigens, with the long-term goal of rapidly and cost-efficiently identifying low-cost vaccine formulations for use in low and middle income countries. Elsevier 2021-03 /pmc/articles/PMC7884052/ /pubmed/33285182 http://dx.doi.org/10.1016/j.xphs.2020.11.039 Text en © 2020 The Authors 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 Research Article
Sawant, Nishant
Kaur, Kawaljit
Holland, David A.
Hickey, John M.
Agarwal, Sanjeev
Brady, Joseph R.
Dalvie, Neil C.
Tracey, Mary Kate
Velez-Suberbie, M. Lourdes
Morris, Stephen A.
Jacob, Shaleem I.
Bracewell, Daniel G.
Mukhopadhyay, Tarit K.
Love, Kerry R.
Love, J. Christopher
Joshi, Sangeeta B.
Volkin, David B.
Rapid Developability Assessments to Formulate Recombinant Protein Antigens as Stable, Low-Cost, Multi-Dose Vaccine Candidates: Case-Study With Non-Replicating Rotavirus (NRRV) Vaccine Antigens
title Rapid Developability Assessments to Formulate Recombinant Protein Antigens as Stable, Low-Cost, Multi-Dose Vaccine Candidates: Case-Study With Non-Replicating Rotavirus (NRRV) Vaccine Antigens
title_full Rapid Developability Assessments to Formulate Recombinant Protein Antigens as Stable, Low-Cost, Multi-Dose Vaccine Candidates: Case-Study With Non-Replicating Rotavirus (NRRV) Vaccine Antigens
title_fullStr Rapid Developability Assessments to Formulate Recombinant Protein Antigens as Stable, Low-Cost, Multi-Dose Vaccine Candidates: Case-Study With Non-Replicating Rotavirus (NRRV) Vaccine Antigens
title_full_unstemmed Rapid Developability Assessments to Formulate Recombinant Protein Antigens as Stable, Low-Cost, Multi-Dose Vaccine Candidates: Case-Study With Non-Replicating Rotavirus (NRRV) Vaccine Antigens
title_short Rapid Developability Assessments to Formulate Recombinant Protein Antigens as Stable, Low-Cost, Multi-Dose Vaccine Candidates: Case-Study With Non-Replicating Rotavirus (NRRV) Vaccine Antigens
title_sort rapid developability assessments to formulate recombinant protein antigens as stable, low-cost, multi-dose vaccine candidates: case-study with non-replicating rotavirus (nrrv) vaccine antigens
topic Research Article
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC7884052/
https://www.ncbi.nlm.nih.gov/pubmed/33285182
http://dx.doi.org/10.1016/j.xphs.2020.11.039
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