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- W2043284863 endingPage "1213" @default.
- W2043284863 startingPage "1193" @default.
- W2043284863 abstract "During the last 20 years, pharmaceutical industry and academic efforts have led to several structurally unrelated classes of non-peptide cholecystokinin-1 receptor (CCK1-R) antagonists. Due to the lack of high resolution structure of CCK1-R and its peptide ligand, different strategies to design antagonists have been adopted. The rational design, based on conformational studies of the endogenous ligand, has provided the so-called ‘peptoid’ derivatives and conformationally restricted peptoids, whereas all of the other non-peptide antagonists derived by empirical and/or conventional approaches, including the chemical manipulation of natural products, disconnection strategies and the use of single key amino acids. All of these strategies include a final optimisation step of the obtained lead compound performed by chemical modifications. The CCK1-R antagonists, in addition to providing a better characterisation of the CCK1-R receptor subtype as pharmacological tools and improving the knowledge of the physiological and pathological role(s) of CCK, may possess therapeutic potential in humans. As the complex biological effects of CCK mediated by CCK1-R in the CNS are not yet completely established, the therapeutic potential of these antagonists at present is limited to the gastrointestinal system disorders. Up until now, loxiglumide and its R-enantiomer (dexloxiglumide) along with lintitript are the CCK1-R antagonists at the most advanced stage of clinical research in gastroenterology." @default.
- W2043284863 created "2016-06-24" @default.
- W2043284863 creator A5034452186 @default.
- W2043284863 creator A5089465265 @default.
- W2043284863 date "2006-08-31" @default.
- W2043284863 modified "2023-10-16" @default.
- W2043284863 title "Twenty years of non-peptide CCK<sub>1</sub>receptor antagonists: all that glitters is not gold" @default.
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