TY - JOUR T1 - Three-dimensional quantitative structure-activity relationship analyses of beta-lactam antibiotics and tripeptides as substrates of the mammalian H+/peptide cotransporter PEPT1. AU - Biegel,Annegret, AU - Gebauer,Sabine, AU - Hartrodt,Bianka, AU - Brandsch,Matthias, AU - Neubert,Klaus, AU - Thondorf,Iris, PY - 2005/6/25/pubmed PY - 2005/8/24/medline PY - 2005/6/25/entrez SP - 4410 EP - 9 JF - Journal of medicinal chemistry JO - J Med Chem VL - 48 IS - 13 N2 - The utilization of the membrane transport protein PEPT1 as a drug delivery system is a promising strategy to enhance the oral bioavailability of drugs. Since very little is known about the substrate binding site of PEPT1, computational methods are a meaningful tool to gain a more detailed insight into the structural requirements for substrates. Three-dimensional quantitative structure-activity relationship (3D-QSAR) studies using the comparative molecular similarity indices analysis (CoMSIA) method were performed on a training set of 98 compounds. Affinity constants of beta-lactam antibiotics and tripeptides were determined at Caco-2 cells. A statistically reliable model of high predictive power was obtained (q(2) = 0.828, r(2) = 0.937). The results derived from CoMSIA were graphically interpreted using different field contribution maps. We identified those regions which are crucial for the interaction between peptidomimetics and PEPT1. The new 3D-QSAR model was used to design a new druglike compound mimicking a dipeptide. The predicted K(i) value was confirmed experimentally. SN - 0022-2623 UR - https://www.unboundmedicine.com/medline/citation/15974593/Three_dimensional_quantitative_structure_activity_relationship_analyses_of_beta_lactam_antibiotics_and_tripeptides_as_substrates_of_the_mammalian_H+/peptide_cotransporter_PEPT1_ DB - PRIME DP - Unbound Medicine ER -