Title: Improving on Nature: Making a Cyclic Heptapeptide Orally Bioavailable.
Authors: Nielsen, Daniel S.; Hoang, Huy N.; Lohman, Rink ‐ Jan; Hill, Timothy A.; Lucke, Andrew J.; Craik, David J.; Edmonds, David J.; Griffith, David A.; Rotter, Charles J.; Ruggeri, Roger B.; Price, David A.; Liras, Spiros; Fairlie, David P.
Abstract: The use of peptides in medicine is limited by low membrane permeability, metabolic instability, high clearance, and negligible oral bioavailability. The prediction of oral bioavailability of drugs relies on physicochemical properties that favor passive permeability and oxidative metabolic stability, but these may not be useful for peptides. Here we investigate effects of heterocyclic constraints, intramolecular hydrogen bonds, and side chains on the oral bioavailability of cyclic heptapeptides. NMR-derived structures, amide H-D exchange rates, and temperature-dependent chemical shifts showed that the combination of rigidification, stronger hydrogen bonds, and solvent shielding by branched side chains enhances the oral bioavailability of cyclic heptapeptides in rats without the need for N-methylation.
Subjects: PEPTIDES; BIOAVAILABILITY; NUCLEAR magnetic resonance; CHEMICAL bonds; C-terminal residues
Publication: Angewandte Chemie, 2014, Vol 126, Issue 45, p12255
ISSN: 0044-8249
Publication type: Academic Journal
DOI: 10.1002/ange.201405364

Improving on Nature: Making a Cyclic Heptapeptide Orally Bioavailable.

Nielsen, Daniel S.; Hoang, Huy N.; Lohman, Rink ‐ Jan; Hill, Timothy A.; Lucke, Andrew J.; Craik, David J.; Edmonds, David J.; Griffith, David A.; Rotter, Charles J.; Ruggeri, Roger B.; Price, David A.; Liras, Spiros; Fairlie, David P.