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新型强效高选择性 5-HT 受体激动剂 YH12852 显著改善上消化道和下消化道运动功能。

The novel, potent and highly selective 5-HT receptor agonist YH12852 significantly improves both upper and lower gastrointestinal motility.

机构信息

Yuhan R&D Institute, Yongin-si, Gyeonggi-do, Republic of Korea.

出版信息

Br J Pharmacol. 2018 Feb;175(3):485-500. doi: 10.1111/bph.14096. Epub 2018 Jan 6.

Abstract

BACKGROUND AND PURPOSE

5-HT receptor agonists have been shown to be effective at treating various gastrointestinal tract disorders. However, a lack of selectivity against off-targets has been a limiting factor for their clinical use.

EXPERIMENTAL APPROACH

The binding affinity and selectivity of YH12852 for human 5-HT receptor in CHO-K1 cells were evaluated using radioligand binding assays, and agonistic activity was assessed using a β-lactamase reporter system. Contractile activity and propulsive motility were measured in the guinea pig isolated distal colon. Its prokinetic effect on the gastrointestinal tract was evaluated in guinea pigs, dogs and monkeys. Its tissue distribution was evaluated in rats.

KEY RESULTS

YH12852 exhibited high affinity and potency for human recombinant 5-HT receptor with high selectivity over other 5-HT and non-5-HT receptors, ion channels, enzymes and transporters. YH12852 induced contractions and increased propulsive motility in guinea pig isolated colon. These effects were abolished by the 5-HT receptor antagonist GR113808. YH12852 increased defecation more effectively than prucalopride in guinea pigs and dogs and improved gastric emptying more effectively than mosapride in guinea pigs, dogs and monkeys. YH12852 was highly distributed to the gastrointestinal tract as the target organ.

CONCLUSION AND IMPLICATIONS

The high in vitro potency and selectivity of YH12852 for 5-HT receptor translated into potent in vivo efficacy with good tolerability. YH12852 significantly improved both upper and lower bowel motility in the animal models tested and has the potential to address considerable unmet needs in patients with functional constipation, gastroparesis or both.

摘要

背景和目的

5-HT 受体激动剂已被证明可有效治疗各种胃肠道疾病。然而,针对非靶点的选择性缺乏一直是其临床应用的限制因素。

实验方法

采用放射性配体结合试验评估 YH12852 在 CHO-K1 细胞中与人 5-HT 受体的结合亲和力和选择性,并采用β-内酰胺酶报告基因系统评估激动活性。在豚鼠离体远端结肠中测量收缩活性和推进运动。在豚鼠、狗和猴子中评估其对胃肠道的促动力作用。在大鼠中评估其组织分布。

主要结果

YH12852 对人重组 5-HT 受体具有高亲和力和效力,对其他 5-HT 和非 5-HT 受体、离子通道、酶和转运体具有高选择性。YH12852 诱导豚鼠离体结肠收缩并增加推进运动。这些作用被 5-HT 受体拮抗剂 GR113808 阻断。YH12852 比普芦卡必利更有效地增加豚鼠和狗的排便,比莫沙必利更有效地改善豚鼠、狗和猴子的胃排空。YH12852 高度分布到胃肠道作为靶器官。

结论和意义

YH12852 对 5-HT 受体具有高体外效力和选择性,转化为具有良好耐受性的有效体内疗效。YH12852 显著改善了在测试动物模型中的上消化道和下消化道运动,并有潜力满足功能性便秘、胃轻瘫或两者兼有的患者的大量未满足需求。

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