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设计、合成及生物评价 17-环丙甲基-3,14β-二羟基-4,5α-环氧-6β-[(4′-吡啶基)羰酰胺基]吗啡喃衍生物作为外周选择性μ阿片受体激动剂。

Design, synthesis, and biological evaluation of 17-cyclopropylmethyl-3,14β-dihydroxy-4,5α-epoxy-6β-[(4'-pyridyl)carboxamido]morphinan derivatives as peripheral selective μ opioid receptor Agents.

机构信息

Department of Medicinal Chemistry, Virginia Commonwealth University , 800 East Leigh Street, Richmond, Virginia 23298, United States.

出版信息

J Med Chem. 2012 Nov 26;55(22):10118-29. doi: 10.1021/jm301247n. Epub 2012 Nov 9.

Abstract

Peripheral selective μ opioid receptor (MOR) antagonists could alleviate the symptoms of opioid-induced constipation (OIC) without compromising the analgesic effect of opioids. However, a variety of adverse effects were associated with them, partially due to their relatively low MOR selectivity. NAP, a 6β-N-4'-pyridyl substituted naltrexamine derivative, was identified previously as a potent and highly selective MOR antagonist mainly acting within the peripheral nervous system. The noticeable diarrhea associated with it prompted the design and synthesis of its analogues in order to study its structure-activity relationship. Among them, compound 8 showed improved pharmacological profiles compared to the original lead, acting mainly at peripheral while increasing the intestinal motility in morphine-pelleted mice (ED(50) = 0.03 mg/kg). The slight decrease of the ED(50) compared to the original lead was well compensated by the unobserved adverse effect. Hence, this compound seems to be a more promising lead to develop novel therapeutic agents toward OIC.

摘要

外周选择性 μ 阿片受体 (MOR) 拮抗剂可缓解阿片类药物引起的便秘 (OIC) 症状,而不影响阿片类药物的镇痛效果。然而,它们与多种不良反应相关,部分原因是其相对较低的 MOR 选择性。NAP 是一种 6β-N-4′-吡啶取代的纳曲胺衍生物,先前被鉴定为一种强效且高度选择性的 MOR 拮抗剂,主要作用于外周神经系统。与其相关的明显腹泻促使设计和合成其类似物,以研究其构效关系。其中,化合物 8 与原始先导化合物相比,显示出改善的药理学特征,主要在外周起作用,同时增加吗啡丸状小鼠的肠道蠕动(ED(50)= 0.03mg/kg)。与原始先导化合物相比,ED(50)略有下降,但未观察到不良反应,因此得到了很好的补偿。因此,该化合物似乎是开发治疗 OIC 新型治疗剂的更有前途的先导化合物。

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