Rational Design, Synthesis, and Pharmacological Characterization of Novel Ghrelin Receptor Inverse Agonists as Potential Treatment against Obesity-Related Metabolic Diseases

Daina Antoine; Giuliano Claudio; Pietra Claudio; Wang Junbo; Chi Yushi; Zou Zack; Li Fugang; Yan Zhonghua; Zhou Yifan; Guainazzi Angelo; Rubio Silvina Garcia; Zoete Vincent

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Rational Design, Synthesis, and Pharmacological Characterization of Novel Ghrelin Receptor Inverse Agonists as Potential Treatment against Obesity-Related Metabolic Diseases

机译：新的Ghrelin受体反向激动剂的理性设计，合成和药理表征作为肥胖相关的代谢疾病的潜在治疗

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A new chemotype of ghrelin inverse agonists was discovered through chimeric design based on molecular scaffolds known as growth-hormone secretagogue receptor (GHSR) modulators but with divergent pharmacodynamic and pharmacokinetic properties. The structure-activities/properties exploration led to compound 47, which displayed potent human GHSR antagonism and inverse agonism in cellular assays (IC50 = 68 nM, EC50 = 29 nM), moderate oral bioavailability, and notable brain penetration in rat (F = 27%, B/P ratio = 1.9). First in vivo studies demonstrated effective reduction of food intake after oral or parenteral administration to mouse (78% at 1 h and 38% at 8 h, respectively). Further preclinical studies are needed to evaluate the most suited mode of administration with the aim of promoting a first central-acting ghrelin inverse agonist molecule to development, which would represent a significant step toward therapeutic agents to treat metabolic disorders related to obesity, such as type 2 diabetes mellitus.

机译：通过基于被称为生长激素促分泌素受体（GHSR）调节剂的分子支架，通过嵌合设计，通过嵌合设计发现了一种新的Ghrelin反向激动剂的嗜型倒出者。结构 - 活动/性质探索导致化合物47，其在细胞测定中显示有效的人类GHSR拮抗作用和反向激动主义（IC50 = 68nm，EC50 = 29nm），中等口服生物利用度，大鼠中的显着脑渗透（F = 27 ％，B / P比率= 1.9）。首先在体内研究证明口服或肠胃外给药后食物摄入的有效减少（分别在8小时的78％和38％）。需要进一步的临床前研究来评估最适合的给药方式，目的是促进第一个中枢神经逆激动剂分子到发育，这将为治疗剂的重要步骤代表治疗与肥胖有关的代谢障碍，例如类型2个糖尿病。

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《Journal of Medicinal Chemistry 》 |2018年第24期| 共22页
作者
Daina Antoine; Giuliano Claudio; Pietra Claudio; Wang Junbo; Chi Yushi; Zou Zack; Li Fugang; Yan Zhonghua; Zhou Yifan; Guainazzi Angelo; Rubio Silvina Garcia; Zoete Vincent;
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作者单位

SIB Mol Modeling Grp CH-1015 Lausanne Switzerland;

Helsinni Healthcare Res &

Preclin Dev Dept CH-6912 Lugano Switzerland;

Helsinni Healthcare Res &

Preclin Dev Dept CH-6912 Lugano Switzerland;

Sundia MediTech Dept Med Chem Pharmacokinet &

Metab 388 Jialilue Rd Zhangjiang Hitech Pk Shanghai 201203 Peoples R China;

Sundia MediTech Dept Med Chem Pharmacokinet &

Metab 388 Jialilue Rd Zhangjiang Hitech Pk Shanghai 201203 Peoples R China;

Sundia MediTech Dept Med Chem Pharmacokinet &

Metab 388 Jialilue Rd Zhangjiang Hitech Pk Shanghai 201203 Peoples R China;

HD Biosci Dept Discovery Biol 590 Ruiqing Rd Zhangjiang East Campus Shanghai 201201 Peoples R China;

HD Biosci Dept Discovery Biol 590 Ruiqing Rd Zhangjiang East Campus Shanghai 201201 Peoples R China;

HD Biosci Dept Discovery Biol 590 Ruiqing Rd Zhangjiang East Campus Shanghai 201201 Peoples R China;

Helsinn Therapeut US Inc Res &

Dev Dept Iselin NJ 08830 USA;

Helsinn Therapeut US Inc Res &

Dev Dept Iselin NJ 08830 USA;

SIB Mol Modeling Grp CH-1015 Lausanne Switzerland;

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正文语种 eng
中图分类药学 ;
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1. Rational Design, Synthesis, and Pharmacological Characterization of Novel Ghrelin Receptor Inverse Agonists as Potential Treatment against Obesity-Related Metabolic Diseases [J] . Daina Antoine, Giuliano Claudio, Pietra Claudio, Journal of Medicinal Chemistry . 2018 ,第24期

机译：新的Ghrelin受体反向激动剂的理性设计，合成和药理表征作为肥胖相关的代谢疾病的潜在治疗
2. Design, synthesis, and pharmacological evaluation of multitarget-directed ligands with both serotonergic subtype 4 receptor (5-HT4R) partial agonist and 5-HT6R antagonist activities, as potential treatment of Alzheimer's disease [J] . Yahiaoui Samir, Hamidouche Katia, Ballandonne Celine, European Journal of Medicinal Chemistry: Chimie Therapeutique . 2016 ,第Null期

机译：具有血清素能亚型4受体（5-HT4R）部分激动剂和5-HT6R拮抗剂活性的多靶标配体的设计，合成和药理学评估，可作为阿尔茨海默氏病的潜在治疗方法
3. Design, Synthesis, and Pharmacological Characterization of 2-(2-Furanyl)thiazolo[5,4-d]pyrimidine-5,7-diamine Derivatives: New Highly Potent A(2A) Adenosine Receptor Inverse Agonists with Antinociceptive Activity [J] . Varano Flavia, Catarzi Daniela, Vincenzi Fabrizio, Journal of Medicinal Chemistry . 2016 ,第23期

机译：设计，合成，和药理学表征的2-（2-呋喃基）噻唑并[5,4-d]嘧啶-5,7-二胺衍生物：具有抗伤害感受活性的新型高效A（2A）腺苷受体逆激动剂。
4. Treatment of Diabetes and Obesity by Rationally Designed Peptide Agonists Functioning at Multiple Metabolic Receptors [C] . Noushafarin Khajavi, Heike Biebermann, Matthias Tschop, ESPE Advanced Seminar in Developmental Endocrinology . 2017

机译：通过在多种代谢受体中起作用的合理设计肽激动剂治疗糖尿病和肥胖症
5. Insights into receptor/ligand specificity: A structural and pharmacological study of inverse agonists and their respective receptors. [D] . Patel, Mira P. 2010

机译：对受体/配体特异性的见解：反向激动剂及其各自受体的结构和药理研究。
6. A Novel in vivo Anti-amnesic Agent Specially Designed to Express Both Acetylcholinesterase (AChE) Inhibitory Serotonergic Subtype 4 Receptor (5-HT4R) Agonist and Serotonergic Subtype 6 Receptor (5-HT6R) Inverse Agonist Activities With a Potential Interest Against Alzheimer’s Disease [O] . Bérénice Hatat, Samir Yahiaoui, Cédric Lecoutey, 2019

机译：一种新型的体内抗记忆删除剂专门设计用于表达乙酰胆碱酯酶（AChE）抑制性血清素能亚型4受体（5-HT4R）激动剂和血清素能亚型6受体（5-HT6R）反向激动剂活性对阿尔茨海默氏症有潜在的兴趣疾病
7. Rational Design, Synthesis, and Pharmacological Characterization of Novel Ghrelin Receptor Inverse Agonists as Potential Treatment against Obesity-Related Metabolic Diseases [O] . -1

机译：新的Ghrelin受体反向激动剂的理性设计，合成和药理表征作为肥胖相关的代谢疾病的潜在治疗

Rational Design, Synthesis, and Pharmacological Characterization of Novel Ghrelin Receptor Inverse Agonists as Potential Treatment against Obesity-Related Metabolic Diseases

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