ABSTRACT
A 1,3,4-benzotriazepine was identified as a suitable lead in our effort toward obtaining a non-peptide parathyroid hormone-1 receptor (PTH1R) antagonist. A process of optimization afforded derivatives displaying nanomolar PTH1R affinity, a representative example of which behaved as a PTH1R antagonist in cell-based cyclic adenosine monophosphate (cAMP) assays, with selectivity over PTH2 receptors.
Subject(s)
Benzazepines/chemical synthesis , Receptor, Parathyroid Hormone, Type 1/antagonists & inhibitors , Animals , Benzazepines/chemistry , Benzazepines/pharmacology , Binding, Competitive , Cell Line , Cell Line, Tumor , Cricetinae , Cricetulus , Cyclic AMP/biosynthesis , Humans , Mice , Radioligand Assay , Recombinant Proteins/antagonists & inhibitors , Structure-Activity RelationshipABSTRACT
Starting from a novel, achiral 1,3,4-benzotriazepine-based CCK2 receptor antagonist, a process of optimization has afforded further compounds of this type that maintain the nanomolar affinity for recombinant, human CCK2 receptors and high selectivity over CCK1 receptors observed in the initial lead but display more potent inhibition of pentagastrin-stimulated gastric acid secretion in vivo. Moreover, this has largely been achieved without altering their potency at wild-type canine and rat receptors, as judged by their displacement of [125I]-BH-CCK-8S in a radioligand binding assay and by their activity in an isolated, perfused rat stomach bioassay, respectively. 2-(5-Cyclohexyl-1-(2-cyclopentyl-2-oxo-ethyl)-2-oxo-1,2-dihydro-3H-1,3,4-benzotriazepin-3-yl)-N-(3-(5-oxo-2,5-dihydro- [1,2,4]oxadiazol-3-yl)-phenyl)-acetamide (47) was identified as the most effective compound stemming from this approach, proving to be a potent inhibitor of pentagastrin-stimulated gastric acid secretion in rats and dogs by intravenous bolus as well as by enteral administration.
Subject(s)
Benzodiazepines/chemical synthesis , Gastric Acid/metabolism , Pentagastrin/pharmacology , Receptor, Cholecystokinin B/antagonists & inhibitors , Administration, Oral , Animals , Benzodiazepines/chemistry , Benzodiazepines/pharmacology , Dogs , Gastric Mucosa/metabolism , Humans , Infusions, Intravenous , Injections, Intravenous , Mice , NIH 3T3 Cells , Radioligand Assay , Rats , Recombinant Proteins/antagonists & inhibitors , Structure-Activity RelationshipABSTRACT
A series of 1,3,4-benzotriazepine-based CCK(2) antagonists have been devised by consideration of the structural features that govern CCK receptor affinity and the receptor subtype selectivity of 1,4-benzodiazepine-based CCK(2) antagonists. In contrast to the latter compounds, these novel 1,3,4-benzotriazepines are achiral, yet they display similar affinity for CCK(2) receptors to the earlier molecules and are highly selective over CCK(1) receptors.
Subject(s)
Benzazepines/chemical synthesis , Receptor, Cholecystokinin A/antagonists & inhibitors , Receptor, Cholecystokinin B/antagonists & inhibitors , Animals , Benzazepines/chemistry , Benzazepines/pharmacology , Benzodiazepines/chemistry , Cell Line , Cricetinae , Cricetulus , Crystallography, X-Ray , Humans , Mice , Molecular Structure , Radioligand Assay , Rats , Receptor, Cholecystokinin A/chemistry , Receptor, Cholecystokinin B/chemistry , Stereoisomerism , Structure-Activity RelationshipABSTRACT
A new molecular modeling approach has been used to derive a pharmacophore of the potent and selective cholecystokinin-2 (CCK(2)) receptor antagonist 5 (JB93182), based on features shared with two related series. The technique uses "field points" as simple and effective descriptions of the electrostatic and van der Waals maxima and minima surrounding a molecule equipped with XED (extended electron distribution) charges. Problems associated with the high levels of biliary elimination of 5 in vivo required us to design a compound with significantly lower molecular weight without sacrificing its nanomolar levels of in vitro activity. Two new series of compounds were designed to mimic the arrangement of field points present in the pharmacophore rather than its structural elements. In a formal sense, two of the three amides in 5 were replaced with either a simple pyrrole or imidazole, while some features thought to be essential for the high levels of in vitro activity of the parent compounds were retained and others deleted. These compounds maintained activity and selectivity for this receptor over CCK(1). In addition, the reduction in molecular weight coupled with lower polarities greatly reduced levels of biliary elimination associated with 5. This makes them good lead compounds for development of drug candidates whose structures are not obviously related to those of the parents and represents the first example of scaffold hopping using molecular field points.
Subject(s)
Imidazoles/chemistry , Models, Molecular , Pyrroles/chemistry , Receptor, Cholecystokinin B/agonists , Receptor, Cholecystokinin B/antagonists & inhibitors , Animals , Binding, Competitive , Cerebral Cortex/metabolism , Drug Design , Imidazoles/chemical synthesis , Imidazoles/pharmacology , In Vitro Techniques , Mice , Molecular Conformation , Pyrroles/chemical synthesis , Pyrroles/pharmacology , Quantitative Structure-Activity Relationship , Radioligand Assay , Receptor, Cholecystokinin B/metabolismABSTRACT
The systematic optimization of the structure of a novel 2,4,5-trisubstituted imidazole-based cholecystokinin-2 (CCK(2)) receptor antagonist afforded analogues with nanomolar receptor affinity. These compounds were now comparable in their potency to the bicyclic heteroaromatic-based compounds 5 (JB93182) and 6 (JB95008), from which the initial examples were designed using a field-point based molecular modeling approach. They were also orally active as judged by their inhibition of pentagastrin stimulated acid secretion in conscious dogs, in contrast to the bicyclic heteroaromatic-based compounds, which were ineffective because of biliary elimination. Increasing the hydrophilicity through replacement of a particular methylene group with an ether oxygen, as in 3-{[5-(adamantan-1-yloxymethyl)-2-cyclohexyl-1H-imidazole-4-carbonyl]amino}benzoic acid (53), had little effect on the receptor affinity but significantly increased the oral potency. Comparison of the plasma pharmacokinetics and the inhibition of pentagastrin-stimulated acid output following bolus intraduodenal administration of both 53 and 6 indicated that 53 was well absorbed, had a longer half-life, and was not subject to the elimination pathways of the earlier series.
Subject(s)
Imidazoles/chemical synthesis , Pyrroles/chemical synthesis , Receptor, Cholecystokinin B/antagonists & inhibitors , Administration, Oral , Animals , Biological Availability , Cerebral Cortex/metabolism , Dogs , Female , Gastric Acid/metabolism , Imidazoles/chemistry , Imidazoles/pharmacology , In Vitro Techniques , Infusions, Intravenous , Mice , Models, Molecular , Pentagastrin/administration & dosage , Pentagastrin/pharmacology , Pyrroles/chemistry , Pyrroles/pharmacology , Quantitative Structure-Activity Relationship , Radioligand AssayABSTRACT
omega-(1H-Imidazol-4-yl)alkane-1-sulfonamides were prepared and found to be potent histamine H(3) receptor antagonists. High receptor affinity and a low difference in the data between the bioassays were achieved with 5-(1H-imidazol-4-yl)pentane-1-sulfonic acid 4-chlorobenzylamide (16). Good in vitro profiles were also obtained for 2-hydroxysulfonamide and vinylsulfonamide analogues. This complements and completes the existing set of imidazole-based sulfonamides and sulfamides.
