Toward Potent Ghrelin Receptor Ligands Based on Trisubstituted 1,2,4-Triazole Structure. 2. Synthesis and Pharmacological in Vitro and in Vivo Evaluations

Moulin, Aline; Demange, Luc; Bergé, Gilbert; Gagne, Didier; Ryan, Joanne; Mousseaux, Delphine; Heitz, Annie; Perrissoud, Daniel; Locatelli, Vittorio; Torsello, Antonio; Galleyrand, Jean Claude; Fehrentz, Jean Alaín; Martinez, Jean

doi:10.1021/jm0704550

Cited by 118 publications

(121 citation statements)

References 11 publications

(26 reference statements)

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“…In this particular situation, detection of partial agonists was problematic because the high basal level of IP1 production might hide the partial agonist character of some ligands. This was the case for JMV 2959, first reported as an antagonist (35,47), but it displayed no or partial agonist activity depending on whether the basal activity was higher or lower than 60% of the maximal ghrelin response. Indeed, we unambiguously highlighted here the partial agonist character of JMV 2959 and of other compounds (JMV 3002 and JMV 3018) by testing their efficacy on the GHS-R1a-A204E mutant, which exhibits a low constitutive activity (42).…”

Section: Discussionmentioning

confidence: 89%

“…Materials and Methods-Ghrelin (35), and JMV 3002, JMV 3018, and JMV 3011 were described previously by Moulin et al (36). In compound JMV 4484, a second chiral center was introduced at position 3 of the 1,2,4-triazole scaffold.…”

Section: Methodsmentioning

confidence: 99%

“…It also remains to be assessed whether the ligand-directed functional selectivity toward downstream signaling pathways leads to a functional selectivity toward physiological functions controlled by the ghrelin/GHS-R1a axis. One can nevertheless point out that in vivo studies in rat demonstrated that JMV 2959 inhibited food intake and addiction but not GH secretion promoted by ghrelin (35,47). This observation is of importance because it suggests that a potential link may exist between the selective action of JMV 2959 toward the signaling pathways activated by GHS-R1a and its selective antagonist action toward physiological responses promoted by ghrelin (Fig.…”

Section: Journal Of Biological Chemistrymentioning

confidence: 96%

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Agonism, Antagonism, and Inverse Agonism Bias at the Ghrelin Receptor Signaling

M’Kadmi

Leyris

Onfroy

et al. 2015

Journal of Biological Chemistry

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107

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Background: GHS-R1a activates multiple signaling pathways mediating feeding and addictive behaviors. Results: Some GHS-R1a ligands activate G q but not G i/o and fail to recruit ␤-arrestin2; others act as selective inverse agonists at G q compared with G 13 . Conclusion: Synthetic ligands can selectively activate or reverse G q -dependent signaling at GHS-R1a. Significance: Ligand-biased signaling can be exploited for the development of selective drugs to treat GHS-R1a-mediated disorders.

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Section: Discussionmentioning

confidence: 89%

Section: Methodsmentioning

confidence: 99%

Section: Journal Of Biological Chemistrymentioning

confidence: 96%

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Agonism, Antagonism, and Inverse Agonism Bias at the Ghrelin Receptor Signaling

M’Kadmi

Leyris

Onfroy

et al. 2015

Journal of Biological Chemistry

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107

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“…Validation using 2 different GHS-R1A antagonists in these models was important because of their different pharmacological profile with respect to food intake. Whereas JMV2959 suppresses food intake by a GHS-R1A agonist (hexarelin) as expected (24,30), BIM28163 paradoxically stimulates food intake (23) via an unknown mechanism that is likely to be independent of GHS-R1A and also independent of ghrelin signaling at the level of the mesolimbic dopaminergic system. Our demonstration that both GHS-R1A antagonists block alcohol intake in a free-choice limited access paradigm together with the absence of ghrelin-induced alcohol consumption in GHS-R1A knockout mice suggests that endogenous ghrelin signaling via GHS-R1A is required for the rewarding properties of alcohol.…”

Section: Discussionmentioning

confidence: 89%

Requirement of central ghrelin signaling for alcohol reward

Jerlhag¹,

Egecioglu

Landgren³

et al. 2009

Proc. Natl. Acad. Sci. U.S.A.

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372

367

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The stomach-derived hormone ghrelin interacts with key CNS circuits regulating energy balance and body weight. Here we provide evidence that the central ghrelin signaling system is required for alcohol reward. Central ghrelin administration (to brain ventricles or to tegmental areas involved in reward) increased alcohol intake in a 2-bottle (alcohol/water) free choice limited access paradigm in mice. By contrast, central or peripheral administration of ghrelin receptor (GHS-R1A) antagonists suppressed alcohol intake in this model. Alcohol-induced locomotor stimulation, accumbal dopamine release and conditioned place preference were abolished in models of suppressed central ghrelin signaling: GHS-R1A knockout mice and mice treated with 2 different GHS-R1A antagonists. Thus, central ghrelin signaling, via GHS-R1A, not only stimulates the reward system, but is also required for stimulation of that system by alcohol. Our data suggest that central ghrelin signaling constitutes a potential target for treatment of alcohol-related disorders.appetite ͉ ethanol ͉ GHS-R1A ͉ mesolimbic dopamine system ͉ reinforcing

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“…Имеются данные об участии грелиновой системы в формировании алкогольной зависимости. Так, введение грелина повышает [12], а блокада грелиновых рецепторов снижает [12,13,16] потребление алкоголя мышами. Предполагается, что эти функции либо опосредова-ны моноаминергической регуляцией, либо реализу-ются через гетеродимерный рецептор GHSR1a/D1R [14,23].…”

Section: Introductionunclassified

The effect of the ghrelin receptors inhibitor [D-Lys3]-GHRP-6 on the levels and metabolism of monoamines in symmetric brain areas of rats treated chronically with alcohol

Karpova

Владимировна²,

Bychkov

et al. 2017

Rev Clin Pharm Drug Ther

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Ключевые слова: антагонист грелина; принудительная хроническая алкоголиза-ция; моноамины; межполушарная асимметрия. РезюмеЦелью исследования было изучить влияния блокады гре-линовых рецепторов GHS-R1a на состояние симметричных моноаминергических систем головного мозга крыс. В частно-сти, предполагалось выяснить, способствует ли применение антагониста грелина [D-Lys 3 ]-GHRP-6 восстановлению ис-ходного содержания моноаминов и их метаболитов в голов-ном мозге животных, хронически потребляющих алкоголь. Методы. Опыты проведены на 22 самцах крыс линии «Ви-стар». Экспериментальные животные вместо питьевой воды получали 10 % раствор этанола. Крысы контрольных групп продолжали потреблять водопроводную воду. Через 6 меся-цев после начала принудительной хронической алкоголиза-ции 6 крысам, получавшим алкоголь, и 6 крысам, получав-шим воду, в течение месяца, раз в три дня, интраназально вводили антагонист грелина [D-Lys 3 ]-GHRP-6 (1 мкг/мкл, по 10 мкл в каждую ноздрю). Остальным животным в том же режиме вводили эквивалентный объем физраствора. Через 80 минут после последнего интраназального введения пре-паратов крыс декапитировали. В гипоталамусе, обонятель-ном бугорке, стриатуме и гиппокампе правой и левой сторон мозга методом ВЭЖХ с электрохимической детекцией опре-деляли содержание норадреналина (НА), дофамина (ДА), диоксифенилуксусной кислоты (ДОФУК), гомованилиновой кислоты (ГВК), серотонина (5-ГТ) и гидроксииндолуксусной кислоты (5-ГИУК). Полученные результаты обрабатывали по t-критерию Стьюдента с использованием пакета статисти-ческих программ GraphPad Prism 6.0. Результаты. У кон-трольных крыс (не подвергавшихся воздействию ни алкоголя, ни препарата) в левом стриатуме обнаружилось достоверное преобладание уровня 5-ГИУК по сравнению с аналогичным показателем другой стороны мозга. Под действием хрониче-ского потребления 10 % раствора этанола исходная левосто-ронняя асимметрия исчезала. Этанол увеличивал содержание 5-ГТ в левом гиппокампе, 5-ГИУК -в правом обонятель-ном бугорке и ДА -в правом гипоталамусе. Препарат

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Toward Potent Ghrelin Receptor Ligands Based on Trisubstituted 1,2,4-Triazole Structure. 2. Synthesis and Pharmacological in Vitro and in Vivo Evaluations

Cited by 118 publications

References 11 publications

Agonism, Antagonism, and Inverse Agonism Bias at the Ghrelin Receptor Signaling

Agonism, Antagonism, and Inverse Agonism Bias at the Ghrelin Receptor Signaling

Requirement of central ghrelin signaling for alcohol reward

The effect of the ghrelin receptors inhibitor [D-Lys3]-GHRP-6 on the levels and metabolism of monoamines in symmetric brain areas of rats treated chronically with alcohol

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