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Literature DB >> 7890609

The role of the cholecystokinin-B/gastrin receptor transmembrane domains in determining affinity for subtype-selective ligands.

A S Kopin¹, E W McBride, S M Quinn, L F Kolakowski, M Beinborn.

Abstract

We have examined the role of transmembrane domain amino acids in conferring subtype-selective ligand affinity to the human cholecystokinin-B (CCK-B)/gastrin receptor. Fifty-eight residues were sequentially replaced by the corresponding amino acids from the pharmacologically distinct CCK-A receptor subtype. 125I-CCK-8 competition binding experiments were performed to compare all mutant CCK-B/gastrin receptor constructs with the wild type control. Affinities for the nonselective agonist, CCK-8, as well as the subtype-selective peptide (gastrin), peptide-derived (PD135,158), and nonpeptide (L365,260) and L364,718) ligands were assessed. All of the mutants retained relatively high affinity for CCK-8, suggesting that the tertiary structure of these receptors was well maintained. Only eight of the amino acid substitutions had a significant effect on subtype selective binding. When compared with the wild type, single point mutations in the CCK-B/gastrin receptor decreased affinity for gastrin, L365,260, and PD135,158 up to 17-,23-, and 61-fold, respectively. In contrast, the affinity for L364,718 increased up to 63-fold. None of the single amino acid substitutions, however, was sufficient to fully account for the subtype selectivity of any tested compound. Rather, CCK-B/gastrin receptor affinity appears to be influenced by multiple residues acting in concert. The 8 pharmacologically important amino acids cluster in the portion of the transmembrane domains adjacent to the cell surface. The spatial orientation of these residues was analyzed with a rhodopsin-based three-dimensional model of G-protein coupled receptor structure (Baldwin, J.M. (1993) EMBO J. 12, 1693-1703). This model predicts that the 8 crucial residues project into a putative ligand pocket, similar to the one which is well established for biogenic amine receptors (Caron, M. G., and Lefkowitz, R.J. (1993) Recent Prog. Horm. Res. 48, 277-290; Strader, C.D., Sigal, I.S., and Dixon, R.A. (1989) Trends Pharmacol. Sci. 10, Dec. Suppl., 26-30).

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Year: 1995 PMID： 7890609 DOI： 10.1074/jbc.270.10.5019

Source DB: PubMed Journal: J Biol Chem ISSN： 0021-9258 Impact factor: 5.157

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Cited

11 in total

1. Identification of a series of CCK-2 receptor nonpeptide agonists: sensitivity to stereochemistry and a receptor point mutation.

Authors: Alan S Kopin; Edward W McBride; Ci Chen; Roger M Freidinger; Duan Chen; Chun-Mei Zhao; Martin Beinborn
Journal: Proc Natl Acad Sci U S A Date: 2003-04-15 Impact factor: 11.205

2. Structural requirements of bitter taste receptor activation.

Authors: Anne Brockhoff; Maik Behrens; Masha Y Niv; Wolfgang Meyerhof
Journal: Proc Natl Acad Sci U S A Date: 2010-06-01 Impact factor: 11.205

3. Novel benzodiazepine photoaffinity probe stereoselectively labels a site deep within the membrane-spanning domain of the cholecystokinin receptor.

Authors: Elizabeth M Hadac; Eric S Dawson; James W Darrow; Elizabeth E Sugg; Terry P Lybrand; Laurence J Miller
Journal: J Med Chem Date: 2006-02-09 Impact factor: 7.446

4. Inter- and intraspecies polymorphisms in the cholecystokinin-B/gastrin receptor alter drug efficacy.

Authors: A S Kopin; E W McBride; M C Gordon; S M Quinn; M Beinborn
Journal: Proc Natl Acad Sci U S A Date: 1997-09-30 Impact factor: 11.205

5. Molecular basis for binding and subtype selectivity of 1,4-benzodiazepine antagonist ligands of the cholecystokinin receptor.

Authors: Erin E Cawston; Polo C H Lam; Kaleeckal G Harikumar; Maoqing Dong; Alicja M Ball; Mary Lou Augustine; Eyup Akgün; Philip S Portoghese; Andrew Orry; Ruben Abagyan; Patrick M Sexton; Laurence J Miller
Journal: J Biol Chem Date: 2012-03-30 Impact factor: 5.157

6. A type 1 cholecystokinin receptor mutant that mimics the dysfunction observed for wild type receptor in a high cholesterol environment.

Authors: Aditya J Desai; Kaleeckal G Harikumar; Laurence J Miller
Journal: J Biol Chem Date: 2014-05-13 Impact factor: 5.157

The role of the cholecystokinin-B/gastrin receptor transmembrane domains in determining affinity for subtype-selective ligands.

1. Identification of a series of CCK-2 receptor nonpeptide agonists: sensitivity to stereochemistry and a receptor point mutation.

2. Structural requirements of bitter taste receptor activation.

3. Novel benzodiazepine photoaffinity probe stereoselectively labels a site deep within the membrane-spanning domain of the cholecystokinin receptor.

4. Inter- and intraspecies polymorphisms in the cholecystokinin-B/gastrin receptor alter drug efficacy.

5. Molecular basis for binding and subtype selectivity of 1,4-benzodiazepine antagonist ligands of the cholecystokinin receptor.

6. A type 1 cholecystokinin receptor mutant that mimics the dysfunction observed for wild type receptor in a high cholesterol environment.

7. Conserved cholecystokinin receptor transmembrane domain IV amino acids confer peptide affinity.

Review 8. Structural basis of cholecystokinin receptor binding and regulation.

Review 9. CCKB/gastrin receptor antagonists: recent advances and potential uses in gastric secretory disorders.

10. Sensitivity of cholecystokinin receptors to membrane cholesterol content.