Use of Small-Molecule Crystal Structures To Address Solubility in a Novel Series of G Protein Coupled Receptor 119 Agonists: Optimization of a Lead and in Vivo Evaluation

Scott, James S.; Birch, Alan M.; Brocklehurst, Katy J.; Broo, Anders; Brown, Hayley S.; Butlin, Roger J.; Clarke, D. S.; Davidsson, Öjvind; Ertan, Anne; Goldberg, Kristin; Groombridge, Sam D.; Hudson, Julian A.; Laber, David; Leach, Andrew G.; MacFaul, Philip A.; McKerrecher, Darren; Pickup, Adrian; Schofield, Paul N.; Svensson, Per H.; Sörme, Pernilla; Teague, Joanne

doi:10.1021/jm300310c

Cited by 63 publications

(56 citation statements)

References 45 publications

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“…G Protein-coupled receptor 119 agonists [16]. Disruption of intermolecular interaction between oxygen of the sulfonyl group and hydrogen of a methyl group in the agonist 5 was reported.…”

Section: Improvement Of Solubility By Disrupting Intermolecular mentioning

confidence: 99%

Improving the Water-Solubility of Compounds by Molecular Modification to Disrupt Crystal Packing

Ishikawa

Hashimoto

2015

The Practice of Medicinal Chemistry

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“…G Protein-coupled receptor 119 agonists [16]. Disruption of intermolecular interaction between oxygen of the sulfonyl group and hydrogen of a methyl group in the agonist 5 was reported.…”

Section: Improvement Of Solubility By Disrupting Intermolecular mentioning

confidence: 99%

Improving the Water-Solubility of Compounds by Molecular Modification to Disrupt Crystal Packing

Ishikawa

Hashimoto

2015

The Practice of Medicinal Chemistry

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“…For these reasons, the development of GPR119 agonists has attracted considerable interest as potential pharmacotherapies for type-2 diabetes and obesity (Cornall et al, 2013;Kang, 2013;Ohishi and Yoshida, 2012). A number of chemically diverse synthetic GPR119 agonists have been developed and characterized (Brocklehurst et al, 2011;Scott et al, 2012;Semple et al, 2008Semple et al, , 2011, with four having advanced to clinical trials (Ohishi and Yoshida, 2012).…”

Section: Introductionmentioning

confidence: 99%

“…In the present study we have investigated the chronic effects of the endogenous GPR119 agonist oleoylethanolamide as well as the synthetic agonists AR-231,453, GSK-1292263, MBX-2982, AZ1, AZ2, and AZ3, as described previously (Brocklehurst et al, 2011;Scott et al, 2012;Semple et al, 2008) and shown in Fig. 1.…”

Section: Introductionmentioning

confidence: 99%

Sustained wash-resistant receptor activation responses of GPR119 agonists

Hothersall

Bussey

Brown

et al. 2015

European Journal of Pharmacology

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G protein-coupled receptor 119 (GPR119) is involved in regulating metabolic homoeostasis, with GPR119 agonists targeted for the treatment of type-2 diabetes and obesity. Using the endogenous agonist oleoylethanolamide and a number of small molecule synthetic agonists we have investigated the temporal dynamics of receptor signalling. Using both a dynamic luminescence biosensor-based assay and an endpoint cAMP accumulation assay we show that agonist-driven desensitization is not a major regulatory mechanism for GPR119 despite robust activation responses, regardless of the agonist used. Temporal analysis of the cAMP responses demonstrated sustained signalling resistant to washout for some, but not all of the agonists tested. Further analysis indicated that the sustained effects of one synthetic agonist AR-231,453 were consistent with a role for slow dissociation kinetics. In contrast, the sustained responses to MBX-2982 and AZ1 appeared to involve membrane deposition. We also detect wash-resistant responses to AR-231,453 at the level of physiologically relevant responses in an endogenous expression system (GLP-1 secretion in GLUTag cells). In conclusion, our findings indicate that in a recombinant expression system GPR119 activation is sustained, with little evidence of pronounced receptor desensitization, and for some ligands persistent agonist responses continue despite removal of excess agonist. This provides novel understanding of the temporal responses profiles of potential drug candidates targetting GPR119, and highlights the importance of carefully examining the the mechanisms through which GPCRs generate sustained responses.

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“…Compared with 12, the (R)-methyl offered no improvement in potency or metabolic stability when combined with either nitrile headgroup (29,30). However, dimethoxy compound 31 gave a small increase in potency and reached the limit of quantification for our standard HLM assay.…”

Section: ■ Results and Discussionmentioning

confidence: 89%

“…We suggest that the introduction of a sulfone may have increased crystal packing, as recently reported for a series of GPR 119 agonists. 29 In addition, both 19 and 23 had markedly improved metabolic stability, with the result that when 23 was studied in vivo, bioavailability improved to 16% (rat in vivo Cl = 22 mL/min/ kg). As a result of these interesting observations, further analogues to investigate the SAR around the dimethoxy and sulfone moieties were studied.…”

Section: ■ Results and Discussionmentioning

confidence: 99%

Pharmacokinetic Benefits of 3,4-Dimethoxy Substitution of a Phenyl Ring and Design of Isosteres Yielding Orally Available Cathepsin K Inhibitors

et al. 2012

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Rational structure-based design has yielded highly potent inhibitors of cathepsin K (Cat K) with excellent physical properties, selectivity profiles, and pharmacokinetics. Compounds with a 3,4-(CH₃O)₂Ph motif, such as 31, were found to have excellent metabolic stability and absorption profiles. Through metabolite identification studies, a reactive metabolite risk was identified with this motif. Subsequent structure-based design of isoteres culminated in the discovery of an optimized and balanced inhibitor (indazole, 38).

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Use of Small-Molecule Crystal Structures To Address Solubility in a Novel Series of G Protein Coupled Receptor 119 Agonists: Optimization of a Lead and in Vivo Evaluation

Cited by 63 publications

References 45 publications

Improving the Water-Solubility of Compounds by Molecular Modification to Disrupt Crystal Packing

Improving the Water-Solubility of Compounds by Molecular Modification to Disrupt Crystal Packing

Sustained wash-resistant receptor activation responses of GPR119 agonists

Pharmacokinetic Benefits of 3,4-Dimethoxy Substitution of a Phenyl Ring and Design of Isosteres Yielding Orally Available Cathepsin K Inhibitors

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