ABSTRACT
Previously we had shown that tripeptidyl trifluoromethyl ketones (TFMKs) possessing an N-terminal diarylacylsulfonamide, such as ICI 200,880 and ICI 200,355, displayed unparalleled protection against the lung damage induced by human neutrophil elastase (HNE) when the inhibitors were administered intratracheally. Since the diarylacylsulfonamides were designed specifically to afford a long residence time in the lung, it was not unexpected that inhibitors from this class of TFMKs were not active when administered orally. Upon evaluating a large number of peptidyl TFMKs possessing a variety of N-terminal groups, several compounds were identified which demonstrated oral activity. Compounds were evaluated for their oral activity by measuring their ability to inhibit the increase in lung weight relative to body weight (Lw/Bw), the increase in red blood cells, and the increase in white blood cells induced by intratracheally administered HNE (100 micrograms/hamster). A number of tripeptidyl trifluoromethyl ketones containing neutral N-terminal groups displayed good oral activity, while those containing basic, acidic, or polar groups did not. Compound 50, possessing an N-terminal 4-(CH3O)C6H4CO group, was particularly effective, reducing Lw/Bw by 77%, red cells by 89%, and white cells by 91% when dosed at 37.5 mg/kg orally. Thus, by modifying the N-terminal group of tripeptidyl TFMKs, inhibitors can be designed which are effective in vivo when administered either orally or intratracheally.
Subject(s)
Dipeptides/chemical synthesis , Enzyme Inhibitors/chemical synthesis , Leukocyte Elastase/antagonists & inhibitors , Administration, Oral , Animals , Body Weight/drug effects , Cricetinae , Dipeptides/pharmacology , Dipeptides/therapeutic use , Enzyme Inhibitors/administration & dosage , Enzyme Inhibitors/therapeutic use , Erythrocyte Count , Hemorrhage/prevention & control , Humans , Leukocyte Count , Leukocyte Elastase/pharmacology , Lung/anatomy & histology , Lung Diseases/prevention & control , Male , Mesocricetus , Molecular Structure , Organ Size/drug effects , Structure-Activity Relationship , Trachea/drug effectsABSTRACT
Using molecular modeling and the information derived from X-ray crystal structures of human neutrophil elastase (HNE) and porcine pancreatic elastase (PPE) complexed to peptidic ligands, we have developed a new series of nonpeptidic inhibitors of HNE, the pyridopyrimidine trifluoromethyl ketones (TFMKs). These bicyclic inhibitors were designed to extend the concept of the related pyridone trifluoromethyl ketones by incorporating a rigidly positioned carbonyl group to participate in a hydrogen bonding interaction with the backbone NH groups of Gly-218 and Gly-219 of the enzyme. In addition, the pyrimidine ring serves as a scaffold to vector substituents toward the S5-S4 subsites of the enzyme's extended binding pocket. Furthermore, the heteroatoms of the pyrimidine ring generally increase the aqueous solubility of the pyridopyrimidines relative to pyridone TFMKs. Pyridopyrimidine TFMKs containing a 6-phenyl substituent afforded potent inhibitors of elastase, and several inhibitors from this class of compounds possessed aqueous solubilities of > 0.1 mg/mL and Ki values of < or = 10 nM.
Subject(s)
Drug Design , Enzyme Inhibitors/chemical synthesis , Ketones/chemical synthesis , Pancreatic Elastase/antagonists & inhibitors , Pyridines/chemical synthesis , Pyrimidines/chemical synthesis , Amino Acid Sequence , Binding Sites , Chemical Phenomena , Chemistry, Physical , Enzyme Inhibitors/pharmacology , Humans , Ketones/pharmacology , Leukocyte Elastase , Models, Molecular , Molecular Sequence Data , Molecular Structure , Pancreatic Elastase/chemistry , Pancreatic Elastase/metabolism , Pyridines/pharmacology , Pyrimidines/pharmacology , Solubility , Structure-Activity RelationshipABSTRACT
A series of peptidyl alpha-ketoheterocycles were synthesized and evaluated for their in vitro inhibition of human neutrophil elastase (HNE). Several heterocycles, including oxazoline and benzoxazole, afforded extremely potent inhibitors of HNE (1p-r) with nanomolar to subnanomolar Ki values. The structure-activity relationships revealed that for compounds with a Ki < 1000 nM potency tends to be positively correlated with the sigma I value of the heterocycle. Furthermore, the results in this study support the hypothesis that, in the covalent enzyme-inhibitor adduct, the azole nitrogen atom of the inhibitor heterocycle participates in a hydrogen-bonding interaction with the active-site His-57.
