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κ 阿片受体激动剂的止痒作用:来自啮齿动物到人类的证据。

Antipruritic Effects of Kappa Opioid Receptor Agonists: Evidence from Rodents to Humans.

机构信息

Center for Substance Abuse Research, Lewis Katz School of Medicine at Temple University, Philadelphia, PA, USA.

出版信息

Handb Exp Pharmacol. 2022;271:275-292. doi: 10.1007/164_2020_420.

Abstract

Centrally administered bombesin induces scratching and grooming in rats. These behaviors were blocked by early benzomorphan kappa opioid receptor (KOR) agonists as reported by Gmerek and Cowan in 1984. This was the first evidence that KORs may be involved in the sensation of itch-like behaviors. Subsequent development of additional animal models for acute and chronic itch has led to important discoveries since then. For example, it was found that (a) gastrin-releasing peptide (GRP), natriuretic polypeptide b and their cognate receptors are keys for the transmission of itch sensation at the spinal cord level, (b) dynorphins (Dyns), the endogenous KOR agonists, work as inhibitory neuromodulators of itch at the spinal cord level, (c) in a mouse model for acute itch, certain KOR antagonists elicit scratching, (d) in mouse models of acute or chronic itch, KOR agonists (e.g., U50,488, nalfurafine, CR 845, nalbuphine) suppress scratching induced by different pruritogens, and (e) nalfurafine, CR 845, and nalbuphine are in the clinic or in clinical trials for pruritus associated with chronic kidney disease and chronic liver disease, as well as pruritus in chronic skin diseases.

摘要

中枢给予脑肠肽会诱发大鼠搔抓和梳理行为。Gmerek 和 Cowan 于 1984 年报道,这些行为可被早期苯吗喃类 κ 阿片受体(KOR)激动剂所阻断。这是 KOR 可能参与痒觉样行为感觉的首个证据。此后,针对急性和慢性瘙痒的其他动物模型的进一步发展,自此产生了重要的发现。例如,研究发现:(a)胃泌素释放肽(GRP)、利尿钠肽 B 及其同源受体是在脊髓水平传递瘙痒感觉的关键;(b)内源性 KOR 激动剂强啡肽(Dyns)作为脊髓水平瘙痒的抑制性神经调质;(c)在急性瘙痒的小鼠模型中,某些 KOR 拮抗剂可诱发搔抓;(d)在急性或慢性瘙痒的小鼠模型中,KOR 激动剂(如 U50,488、纳呋拉啡、CR 845、纳布啡)可抑制不同致痒原诱导的搔抓;(e)纳呋拉啡、CR 845 和纳布啡已用于治疗慢性肾脏病和慢性肝病相关瘙痒以及慢性皮肤病瘙痒。

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