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首页> 外文期刊>Regulatory peptides. >Novel endomorphin analogues with antagonist activity at the mu-opioid receptor in the gastrointestinal tract.
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Novel endomorphin analogues with antagonist activity at the mu-opioid receptor in the gastrointestinal tract.

机译:在胃肠道的μ阿片受体上具有拮抗活性的新型内啡肽类似物。

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Opioid bowel dysfunction (OBD) summarizes common adverse side effects of opiate-based management of pain. A promising therapeutic approach to prevent OBD and other opioid-related disorders of the gastrointestinal (GI) tract is the co-administration of opiates with peripherally-restricted mu-opioid receptor (MOR)-selective antagonists. The aim of this study was to investigate the selectivity and efficacy of three novel peptide antagonists: antanal-1, antanal-2, and antanal-2A at MOR in the GI tract in vitro and in vivo. The effects of the antanals on GI motility were studied in vitro, using isolated preparations of mouse ileum and colon and in vivo, by measuring colonic propulsion in mice. Additionally, in vitro stability against enzymatic degradation and blood-brain barrier (BBB) permeability using the hot plate test in mice were examined. The antanals significantly reduced the inhibitory effect of the MOR agonists endomorphin-2, morphine, and loperamide on mouse ileum and colon contractions in vitro and blocked morphine-induced decrease of colonic bead expulsion in vivo. The hot plate test in mice showed that the antagonist activity of all antanals was restricted to the periphery. Antanal-1, antanal-2, and antanal-2A are promising MOR antagonists with limited BBB permeability, which may be developed into future therapeutics of opioid-related GI dysfunction.
机译:阿片类药物肠道功能障碍(OBD)总结了基于鸦片的疼痛管理的常见不良副作用。预防OBD和其他与胃肠道(GI)的阿片类相关疾病的有前途的治疗方法是将阿片类药物与外周限制性mu阿片受体(MOR)选择性拮抗剂并用。这项研究的目的是研究在体外和体内胃肠道中三种新型肽拮抗剂:antanal-1,antanal-2和antanal-2A在MOR的选择性和功效。使用分离的小鼠回肠和结肠制剂以及体外,通过测量小鼠的结肠推进力,研究了蒽类化合物对胃肠动力的影响。另外,使用热板试验在小鼠中检查了针对酶促降解和血脑屏障(BBB)渗透性的体外稳定性。蒽类药物显着降低了MOR激动剂endomorphin-2,吗啡和洛哌丁胺在体外对小鼠回肠和结肠收缩的抑制作用,并在体内阻止了吗啡诱导的结肠珠排出的减少。在小鼠中进行的热板测试表明,所有金属拮抗剂的拮抗活性都局限于周围。 Antanal-1,antanal-2和antanal-2A是有前途的MOR拮抗剂,其BBB通透性有限,可能会发展成为阿片类药物相关胃肠功能障碍的未来治疗方法。

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