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通过靶向痛敏抑制素的分子进行疼痛调节:G蛋白偶联受体与痛敏抑制素相互作用蛋白

Pain regulation by nocistatin-targeting molecules: G protein-coupled-receptor and nocistatin-interacting protein.

作者信息

Okuda-Ashitaka Emiko, Ito Seiji

机构信息

Department of Biomedical Engineering, Osaka Institute of Technology, Osaka, Japan.

Department of Medical Chemistry, Kansai Medical University, Hirakata, Japan.

出版信息

Vitam Horm. 2015;97:147-65. doi: 10.1016/bs.vh.2014.12.001. Epub 2015 Jan 14.

Abstract

Nociceptin/orphanin FQ (N/OFQ) and nocistatin (NST) are neuropeptides produced from the same precursor protein. N/OFQ is involved in a broad range of central functions including pain, learning, memory, anxiety, and feeding. However, NST has opposite effects on various central functions evoked by N/OFQ. The regulation of their receptors may be important for these opposite functions of NST and N/OFQ. Although N/OFQ binds to a specific N/OFQ receptor, the target molecule of NST remains unclear. Some biological effects of NST are mediated by a G protein-coupled receptor. Furthermore, using high-performance affinity nanobeads, we recently identified a 4-nitrophenylphosphatase domain and nonneuronal SNAP25-like protein homolog 1 (NIPSNAP1) as a protein that interacts with NST in the mouse spinal cord. The inhibition of N/OFQ-evoked tactile pain allodynia by NST is mediated by NIPSNAP1. This review focuses on the molecular mechanisms of pain regulation by the target molecules of NST including a G protein-coupled receptor and NIPSNAP1.

摘要

痛敏肽/孤啡肽FQ(N/OFQ)和痛抑素(NST)是由同一前体蛋白产生的神经肽。N/OFQ参与广泛的中枢功能,包括疼痛、学习、记忆、焦虑和进食。然而,NST对N/OFQ引发的各种中枢功能具有相反的作用。它们受体的调节对于NST和N/OFQ的这些相反功能可能很重要。虽然N/OFQ与特定的N/OFQ受体结合,但NST的靶分子仍不清楚。NST的一些生物学效应由G蛋白偶联受体介导。此外,我们最近使用高性能亲和纳米珠,在小鼠脊髓中鉴定出一种4-硝基苯磷酸酶结构域和非神经元SNAP25样蛋白同源物1(NIPSNAP1)作为与NST相互作用的蛋白。NST对N/OFQ诱发的触觉痛觉过敏的抑制作用由NIPSNAP1介导。本综述重点关注包括G蛋白偶联受体和NIPSNAP1在内的NST靶分子对疼痛调节的分子机制。

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