Bioorganic & Medicinal Chemistry Letters 2007-04-01

Comparison of the in vitro apparent permeability and stability of opioid mimetic compounds with that of the native peptide.

Yasuko Koda, Kimitaka Shiotani, Istvan Toth, Yuko Tsuda, Yoshio Okada, Joanne T Blanchfield

Index: Bioorg. Med. Chem. Lett. 17 , 2043-6, (2007)

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Abstract

Three dimethyl-L-tyrosine (Dmt) based peptide analogues were identified in a previous study as excellent agonists for the mu-opioid receptor showing very low K(i) values and good in vivo antinociceptive activity upon intracerebroventricular administration to mice. This activity decreased markedly when the compounds were delivered subcutaneously or orally. To establish the cause of this decrease of activity the apparent permeability across Caco-2 cell monolayers of each compound and their relative stability to the digestive enzymes present in the cell line has been determined and compared to that of the native peptide endomorphin 2. The compounds' permeabilities clearly correlate with their increasing lipophilicity suggesting that the analogues cross the monolayer via passive diffusion and the results show that the compound with high K(i) value for the mu-receptor (K(i)mu=0.114 nM) exhibited the highest permeability suggesting that this may be the better lead compound despite the lower binding affinity than that of compound 2 or 3.


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