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Literature DB >> 30068735

Identification of Positive Allosteric Modulators of the D₁ Dopamine Receptor That Act at Diverse Binding Sites.

Kathryn D Luderman¹, Jennie L Conroy¹, R Benjamin Free¹, Noel Southall¹, Marc Ferrer¹, Marta Sanchez-Soto¹, Amy E Moritz¹, Blair K A Willette¹, Tim J Fyfe¹, Prashi Jain¹, Steve Titus¹, Lisa A Hazelwood¹, Jeffrey Aubé¹, J Robert Lane¹, Kevin J Frankowski¹, David R Sibley².

Abstract

The D1 dopamine receptor is linked to a variety of neuropsychiatric disorders and represents an attractive drug target for the enhancement of cognition in schizophrenia, Alzheimer disease, and other disorders. Positive allosteric modulators (PAMs), with their potential for greater selectivity and larger therapeutic windows, may represent a viable drug development strategy, as orthosteric D1 receptor agonists possess known clinical liabilities. We discovered two structurally distinct D1 receptor PAMs, MLS6585 and MLS1082, via a high-throughput screen of the NIH Molecular Libraries program small-molecule library. Both compounds potentiate dopamine-stimulated G protein- and β-arrestin-mediated signaling and increase the affinity of dopamine for the D1 receptor with low micromolar potencies. Neither compound displayed any intrinsic agonist activity. Both compounds were also found to potentiate the efficacy of partial agonists. We tested maximally effective concentrations of each PAM in combination to determine if the compounds might act at separate or similar sites. In combination, MLS1082 + MLS6585 produced an additive potentiation of dopamine potency beyond that caused by either PAM alone for both β-arrestin recruitment and cAMP accumulation, suggesting diverse sites of action. In addition, MLS6585, but not MLS1082, had additive activity with the previously described D1 receptor PAM "Compound B," suggesting that MLS1082 and Compound B may share a common binding site. A point mutation (R130Q) in the D1 receptor was found to abrogate MLS1082 activity without affecting that of MLS6585, suggesting this residue may be involved in the binding/activity of MLS1082 but not that of MLS6585. Together, MLS1082 and MLS6585 may serve as important tool compounds for the characterization of diverse allosteric sites on the D1 receptor as well as the development of optimized lead compounds for therapeutic use. U.S. Government work not protected by U.S. copyright.

Entities: Chemical Disease Mutation

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Year: 2018 PMID： 30068735 PMCID： PMC6117505 DOI： 10.1124/mol.118.113175

Source DB: PubMed Journal: Mol Pharmacol ISSN： 0026-895X Impact factor: 4.436

30 in total

1. Enhancement of working memory in aged monkeys by a sensitizing regimen of dopamine D1 receptor stimulation.

Authors: Stacy A Castner; Patricia S Goldman-Rakic
Journal: J Neurosci Date: 2004-02-11 Impact factor: 6.167

Review 2. Neurobiology of executive functions: catecholamine influences on prefrontal cortical functions.

Authors: Amy F T Arnsten; Bao-Ming Li
Journal: Biol Psychiatry Date: 2005-06-01 Impact factor: 13.382

3. Inverted-U dopamine D1 receptor actions on prefrontal neurons engaged in working memory.

Authors: Susheel Vijayraghavan; Min Wang; Shari G Birnbaum; Graham V Williams; Amy F T Arnsten
Journal: Nat Neurosci Date: 2007-02-04 Impact factor: 24.884

Review 4. Allosteric modulation of G protein-coupled receptors.

Authors: Lauren T May; Katie Leach; Patrick M Sexton; Arthur Christopoulos
Journal: Annu Rev Pharmacol Toxicol Date: 2007 Impact factor: 13.820

5. Identification of G protein-biased agonists that fail to recruit β-arrestin or promote internalization of the D1 dopamine receptor.

Authors: Jennie L Conroy; R Benjamin Free; David R Sibley
Journal: ACS Chem Neurosci Date: 2015-02-20 Impact factor: 4.418

6. Dose-dependent effects of the dopamine D1 receptor agonists A77636 or SKF81297 on spatial working memory in aged monkeys.

Authors: J X Cai; A F Arnsten
Journal: J Pharmacol Exp Ther Date: 1997-10 Impact factor: 4.030

7. Dihydrexidine, a novel full efficacy D1 dopamine receptor agonist.

Authors: D M Mottola; W K Brewster; L L Cook; D E Nichols; R B Mailman
Journal: J Pharmacol Exp Ther Date: 1992-07 Impact factor: 4.030

Review 8. Targeting the dopamine D1 receptor in schizophrenia: insights for cognitive dysfunction.

Authors: Patricia S Goldman-Rakic; Stacy A Castner; Torgny H Svensson; Larry J Siever; Graham V Williams
Journal: Psychopharmacology (Berl) Date: 2004-04-30 Impact factor: 4.530

Review 9. Allosteric GPCR modulators: taking advantage of permissive receptor pharmacology.

Authors: Katie Leach; Patrick M Sexton; Arthur Christopoulos
Journal: Trends Pharmacol Sci Date: 2007-07-13 Impact factor: 14.819

10. An Allosteric Potentiator of the Dopamine D1 Receptor Increases Locomotor Activity in Human D1 Knock-In Mice without Causing Stereotypy or Tachyphylaxis.

Authors: Kjell A Svensson; Beverly A Heinz; John M Schaus; James P Beck; Junliang Hao; Joseph H Krushinski; Matthew R Reinhard; Michael P Cohen; Sarah L Hellman; Brian G Getman; Xushan Wang; Michelle M Menezes; Deanna L Maren; Julie F Falcone; Wesley H Anderson; Rebecca A Wright; S Michelle Morin; Kelly L Knopp; Benjamin L Adams; Borys Rogovoy; Ilya Okun; Todd M Suter; Michael A Statnick; Donald R Gehlert; David L Nelson; Virginia L Lucaites; Renee Emkey; Neil W DeLapp; Todd R Wiernicki; Jeffrey W Cramer; Charles R Yang; Robert F Bruns
Journal: J Pharmacol Exp Ther Date: 2016-11-03 Impact factor: 4.030

6 in total

Identification of Positive Allosteric Modulators of the D₁ Dopamine Receptor That Act at Diverse Binding Sites.

1. Enhancement of working memory in aged monkeys by a sensitizing regimen of dopamine D1 receptor stimulation.

Review 2. Neurobiology of executive functions: catecholamine influences on prefrontal cortical functions.

3. Inverted-U dopamine D1 receptor actions on prefrontal neurons engaged in working memory.

Review 4. Allosteric modulation of G protein-coupled receptors.

5. Identification of G protein-biased agonists that fail to recruit β-arrestin or promote internalization of the D1 dopamine receptor.

6. Dose-dependent effects of the dopamine D1 receptor agonists A77636 or SKF81297 on spatial working memory in aged monkeys.

7. Dihydrexidine, a novel full efficacy D1 dopamine receptor agonist.

Review 8. Targeting the dopamine D1 receptor in schizophrenia: insights for cognitive dysfunction.

Review 9. Allosteric GPCR modulators: taking advantage of permissive receptor pharmacology.

10. An Allosteric Potentiator of the Dopamine D1 Receptor Increases Locomotor Activity in Human D1 Knock-In Mice without Causing Stereotypy or Tachyphylaxis.

1. Polymer-Modified Carbon Fiber Microelectrodes for Neurochemical Detection of Dopamine and Metabolites.

Review 2. The Impact of the Secondary Binding Pocket on the Pharmacology of Class A GPCRs.

3. Development of pyrimidone D1 dopamine receptor positive allosteric modulators.

4. Enantioenriched Positive Allosteric Modulators Display Distinct Pharmacology at the Dopamine D₁ Receptor.

5. Cell specific photoswitchable agonist for reversible control of endogenous dopamine receptors.

6. Pharmacokinetics of ASP4345 from Single Ascending-Dose and Multiple Ascending-Dose Phase I Studies.