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首页> 外文期刊>Bioorganic and medicinal chemistry >Endomorphin analogues with mixed μ-opioid (MOP) receptor agonism/δ-opioid (DOP) receptor antagonism and lacking β-arrestin2 recruitment activity
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Endomorphin analogues with mixed μ-opioid (MOP) receptor agonism/δ-opioid (DOP) receptor antagonism and lacking β-arrestin2 recruitment activity

机译:内啡肽类似物具有混合的μ阿片类药物(MOP)受体激动作用/δ-阿片类药物(DOP)受体拮抗作用且缺乏β-arrestin2募集活性

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摘要

Analogues of endomorphin (Dmt-Pro-Xaa-Xaa-NH2) modified at position 4 or at positions 4 and 3, and tripeptides (Dmt-Pro-Xaa-NH2) modified at position 3, with various phenylalanine analogues (Xaa = Trp, 1-Nal, 2-Nal, Tmp, Dmp, Dmt) were synthesized and their effects on in vitro opioid activity were investigated. Most of the peptides exhibited high μ-opioid (MOP) receptor binding affinity (KiMOP = 0.13-0.81 nM), modest MOP-selectivity (Kiδ-opioid (DOP)/K iMOP = 3.5-316), and potent functional MOP agonism (GPI, IC 50 = 0.274-249 nM) without DOP and κ-opioid (KOP) receptor agonism. Among them, compounds 7 (Dmt-Pro-Tmp-Tmp-NH2) and 9 (Dmt-Pro-1-Nal-NH2) were opioids with potent mixed MOP receptor agonism/DOP receptor antagonism and devoid of β-arrestin2 recruitment activity. They may offer a unique template for the discovery of potent analgesics that produce less respiratory depression, less gastrointestinal dysfunction and that have a lower propensity to induce tolerance and dependence compared with morphine.
机译:在4位或4位和3位修饰的内啡肽(Dmt-Pro-Xaa-Xaa-NH2)和在3位修饰的三肽(Dmt-Pro-Xaa-NH2)与各种苯丙氨酸类似物(Xaa = Trp,合成了1-Nal,2-Nal,Tmp,Dmp,Dmt),并研究了它们对体外阿片样物质活性的影响。大多数肽表现出高的μ阿片类药物(MOP)受体结合亲和力(KiMOP = 0.13-0.81 nM),适度的MOP选择性(Kiδ-阿片类药物(DOP)/ K iMOP = 3.5-316)和有效的功能性MOP激动作用( GPI,IC 50 = 0.274-249 nM),无DOP和κ阿片类药物(KOP)受体激动作用。其中,化合物7(Dmt-Pro-Tmp-Tmp-NH2)和化合物9(Dmt-Pro-1-Nal-NH2)为类鸦片,具有强效的MOP受体激动/ DOP受体拮抗作用,且无β-arrestin2募集活性。它们可能为发现强效镇痛药提供独特的模板,该镇痛药与吗啡相比,产生的呼吸抑制作用较小,胃肠道功能障碍较少,并且诱导耐受性和依赖性的倾向性较低。

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