Half-life extension and non-human primate pharmacokinetic safety studies of i-body AD-114 targeting human CXCR4

Single domain antibodies that combine antigen specificity with high tissue penetration are an attractive alternative to conventional antibodies. However, rapid clearance from the bloodstream owing to their small size can be a limitation of therapeutic single domain antibodies. Here, we describe and...

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Autores principales: Griffiths, Katherine, Binder, Uli, McDowell, William, Tommasi, Rita, Frigerio, Mark, Darby, William G., Hosking, Chris G., Renaud, Lionel, Machacek, Matthias, Lloyd, Peter, Skerra, Arne, Foley, Michael
Formato: Online Artículo Texto
Lenguaje:English
Publicado: Taylor & Francis 2019
Materias:
Report
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC6748587/
https://www.ncbi.nlm.nih.gov/pubmed/31156041
http://dx.doi.org/10.1080/19420862.2019.1626652
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author Griffiths, Katherine
Binder, Uli
McDowell, William
Tommasi, Rita
Frigerio, Mark
Darby, William G.
Hosking, Chris G.
Renaud, Lionel
Machacek, Matthias
Lloyd, Peter
Skerra, Arne
Foley, Michael
author_facet Griffiths, Katherine
Binder, Uli
McDowell, William
Tommasi, Rita
Frigerio, Mark
Darby, William G.
Hosking, Chris G.
Renaud, Lionel
Machacek, Matthias
Lloyd, Peter
Skerra, Arne
Foley, Michael
author_sort Griffiths, Katherine
collection PubMed
description Single domain antibodies that combine antigen specificity with high tissue penetration are an attractive alternative to conventional antibodies. However, rapid clearance from the bloodstream owing to their small size can be a limitation of therapeutic single domain antibodies. Here, we describe and evaluate the conjugation of a single domain i-body, AD-114, which targets CXCR4, to a panel of half-life extension technologies including a human serum albumin-binding peptide, linear and branched PEG, and PASylation (PA600). The conjugates were assessed in murine, rat and cynomolgus monkey pharmacokinetic studies and showed that the branched PEG was most effective at extending circulating half-life in mice; however, manufacturing limitations of PEGylated test material precluded scale-up and assessment in larger animals. PA600, by comparison, was amenable to scale-up and afforded considerable half-life improvements in mice, rats and cynomolgus monkeys. In mice, the circulating half-life of AD-114 was extended from 0.18 h to 7.77 h following conjugation to PA600, and in cynomolgus monkeys, the circulating half-life of AD-114-PA600 was 24.27 h. AD-114-PA600 was well tolerated in cynomolgus monkeys at dose rates up to 100 mg/kg with no mortalities or drug-related clinical signs.
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spelling pubmed-67485872019-09-25 Half-life extension and non-human primate pharmacokinetic safety studies of i-body AD-114 targeting human CXCR4 Griffiths, Katherine Binder, Uli McDowell, William Tommasi, Rita Frigerio, Mark Darby, William G. Hosking, Chris G. Renaud, Lionel Machacek, Matthias Lloyd, Peter Skerra, Arne Foley, Michael MAbs Report Single domain antibodies that combine antigen specificity with high tissue penetration are an attractive alternative to conventional antibodies. However, rapid clearance from the bloodstream owing to their small size can be a limitation of therapeutic single domain antibodies. Here, we describe and evaluate the conjugation of a single domain i-body, AD-114, which targets CXCR4, to a panel of half-life extension technologies including a human serum albumin-binding peptide, linear and branched PEG, and PASylation (PA600). The conjugates were assessed in murine, rat and cynomolgus monkey pharmacokinetic studies and showed that the branched PEG was most effective at extending circulating half-life in mice; however, manufacturing limitations of PEGylated test material precluded scale-up and assessment in larger animals. PA600, by comparison, was amenable to scale-up and afforded considerable half-life improvements in mice, rats and cynomolgus monkeys. In mice, the circulating half-life of AD-114 was extended from 0.18 h to 7.77 h following conjugation to PA600, and in cynomolgus monkeys, the circulating half-life of AD-114-PA600 was 24.27 h. AD-114-PA600 was well tolerated in cynomolgus monkeys at dose rates up to 100 mg/kg with no mortalities or drug-related clinical signs. Taylor & Francis 2019-08-23 /pmc/articles/PMC6748587/ /pubmed/31156041 http://dx.doi.org/10.1080/19420862.2019.1626652 Text en © 2019 The Author(s). Published with license by Taylor & Francis Group, LLC. http://creativecommons.org/licenses/by-nc-nd/4.0/ This is an Open Access article distributed under the terms of the Creative Commons Attribution-NonCommercial-NoDerivatives License (http://creativecommons.org/licenses/by-nc-nd/4.0/), which permits non-commercial re-use, distribution, and reproduction in any medium, provided the original work is properly cited, and is not altered, transformed, or built upon in any way.
spellingShingle Report
Griffiths, Katherine
Binder, Uli
McDowell, William
Tommasi, Rita
Frigerio, Mark
Darby, William G.
Hosking, Chris G.
Renaud, Lionel
Machacek, Matthias
Lloyd, Peter
Skerra, Arne
Foley, Michael
Half-life extension and non-human primate pharmacokinetic safety studies of i-body AD-114 targeting human CXCR4
title Half-life extension and non-human primate pharmacokinetic safety studies of i-body AD-114 targeting human CXCR4
title_full Half-life extension and non-human primate pharmacokinetic safety studies of i-body AD-114 targeting human CXCR4
title_fullStr Half-life extension and non-human primate pharmacokinetic safety studies of i-body AD-114 targeting human CXCR4
title_full_unstemmed Half-life extension and non-human primate pharmacokinetic safety studies of i-body AD-114 targeting human CXCR4
title_short Half-life extension and non-human primate pharmacokinetic safety studies of i-body AD-114 targeting human CXCR4
title_sort half-life extension and non-human primate pharmacokinetic safety studies of i-body ad-114 targeting human cxcr4
topic Report
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC6748587/
https://www.ncbi.nlm.nih.gov/pubmed/31156041
http://dx.doi.org/10.1080/19420862.2019.1626652
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