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Review
. 2018 Jun 1;26(10):2766-2773.
doi: 10.1016/j.bmc.2017.08.031. Epub 2017 Aug 31.

Improving oral bioavailability of cyclic peptides by N-methylation

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Free article
Review

Improving oral bioavailability of cyclic peptides by N-methylation

Andreas F B Räder et al. Bioorg Med Chem. .
Free article

Abstract

The renaissance of peptides in pharmaceutical industry results from their importance in many biological functions. However, low metabolic stability and the lack of oral availability of most peptides is a certain limitation. Whereas metabolic instability may be often overcome by development of small cyclic peptides containing d-amino acids, the very low oral availability of most peptides is a serious limitation for some medicinal applications. The situation is complicated because a twofold optimization - biological activity and oral availability - is required to overcome this problem. Moreover, most simple "rules" for achieving oral availability are not general and are applicable only to limited cases. Many structural modifications for increasing biological activities and metabolic stabilities of cyclic peptides have been described, of which N-alkylation is probably the most common. This mini-review focuses on the effects of N-methylation of cyclic peptides in strategies to optimize bioavailabilities.

Keywords: Bioavailability; Caco-2; Cyclic peptides; Cyclosporin A; Membrane transport; N-Methylation; Peptide-based drugs; Peptidomimetics.

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