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Half‐life prolongation of therapeutic proteins by conjugation to ATIII ‐binding pentasaccharides: a first‐in‐human study of C arbo C arrier ® insulin
Author(s) -
Miltenburg André M. M.,
Prohn Marita,
Kuijk Jacqueline H. M.,
Tiessen Renger G.,
Kort Martin,
Berg Rob J. W.
Publication year - 2013
Publication title -
british journal of clinical pharmacology
Language(s) - English
Resource type - Journals
SCImago Journal Rank - 1.216
H-Index - 146
eISSN - 1365-2125
pISSN - 0306-5251
DOI - 10.1111/j.1365-2125.2012.04460.x
Subject(s) - insulin , pharmacokinetics , tolerability , pharmacology , pharmacodynamics , chemistry , medicine , endocrinology , half life , adverse effect
Aim Conjugation to antithrombin III ATIII ‐binding pentasaccharides has been proposed as a novel method to extend the half‐life of therapeutic proteins. We aim to validate this technological concept in man by performing a first‐in‐human study using C arbo C arrier® insulin (SCH 900948) as an example. A rising single dose phase 1 study was performed assessing safety, tolerability, pharmacokinetics and relative bioactivity of C arbo C arrier® insulin. Safety, tolerability and pharmacokinetics ( PK ) of single doses of C arbo C arrier® insulin in healthy volunteers were explored, and the dose–response relationship and relative bioactivity of Ca rbo C arrier® insulin in subjects with type 2 diabetes were investigated. Methods After an overnight fast, subjects were randomized to a treatment sequence. PK and pharmacodynamic (glucose, insulin and C ‐peptide) samples were obtained for up to 72 h post‐dose. Effects of C arbo C arrier® insulin were compared with those of NPH ‐insulin. Results C arbo C arrier® insulin was safe and well‐tolerated and no consistent pattern of adverse events occurred. C arbo C arrier® insulin exposure ( C max and AUC ) increased proportionally with dose. The mean terminal elimination half‐life ranged between 3.11 and 5.28 h. All C arbo C arrier® insulin dose groups showed decreases in the mean change from baseline of plasma glucose concentrations compared with the placebo group. Conclusions C arbo C arrier® insulin is pharmacologically active showing features of insulin action in man. The elimination half‐life of the molecule was clearly extended compared with endogenous insulin, indicating that conjugation to ATIII ‐binding pentasaccharides is a viable approach to extend the half‐life of therapeutic proteins in humans. This is an important step towards validation of the C arbo C arrier® technology by making use of C arbo C arrier® insulin as an example.