Issue 5, 2010

Strategies to prolong the plasma residence time of peptidedrugs

Abstract

Peptides are an attractive class of molecules for the development of therapeutics because they combine unique properties such as high binding affinity, excellent target specificity, low toxicity and a relatively small mass. However, the short in vivo half-life of peptides which is typically only a few minutes had hampered the development of a larger number of peptide leads into drugs. The main reasons for the fast elimination of peptides from the circulation are enzymatic degradation and/or fast renal clearance. To prolong the half-life of peptides, their proteolytic stability can be improved by chemical modification strategies and the rate of clearance can be reduced by conjugating the peptides to molecules that prevent their elimination through the kidney. In this article we review the latter class of strategies that aims at prolonging the in vivo plasma residence time of peptides. Techniques including peptidedrug linkage to large polymers, fusion to long-lived proteins such as albumin or the Fc fragment of immunoglobulin and conjugation to small molecule albumin-binding tags are discussed and the peptide-conjugate half-lives achieved are compared.

Graphical abstract: Strategies to prolong the plasma residence time of peptide drugs

Article information

Article type
Review Article
Submitted
15 Jul 2010
Accepted
13 Sep 2010
First published
21 Oct 2010

Med. Chem. Commun., 2010,1, 319-324

Strategies to prolong the plasma residence time of peptidedrugs

L. Pollaro and C. Heinis, Med. Chem. Commun., 2010, 1, 319 DOI: 10.1039/C0MD00111B

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