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首页> 外文期刊>Neuropeptides: An International Journal >Characterization of Substance P processing in mouse spinal cord S9 fractions using high-resolution Quadrupole-Orbitrap mass spectrometry
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Characterization of Substance P processing in mouse spinal cord S9 fractions using high-resolution Quadrupole-Orbitrap mass spectrometry

机译:使用高分辨率高压 - 横射质谱法鉴定小鼠脊髓S9级分体P.

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摘要

Tachykinins are a family of pronociceptive neuropeptides with a specific role in pain and inflammation. Several mechanisms regulate endogenous tachykinins and Substance P (SP) levels, including the differential expression of protachykinin mRNA and the controlled secretion of tachykinins from neurons. Proteolysis is suspected to regulate extracellular SP concentrations but few studies were conducted on the metabolism of proneuropeptides and neuropeptides. Here, we provide evidence that proteolysis controls SP levels in the spinal cord leading to the formation of active C-terminal fragments. Using high-resolution mass spectrometry, specific tachykinins fragments were characterized and quantified. The metabolic stability of beta-Tachykinin(58-71) and SP were very short resulting in half-life of 5.7 and 3.5 min respectively. Several C-terminal fragments were identified, including SP3-11, SP5-11 and SP8-11, which conserve affinity for the Neurokinin 1 receptor. Interestingly, the metabolic stability of C-terminal fragments was significantly superior. Two specific Prolyl endopeptidase inhibitors were used and showed a significant reduction in the rate of formation of SP3-11 and SP5-11 providing strong evidence that Prolyl endopeptidase is involved into N-terminal processing of SP in the spinal cord. (C) 2016 Elsevier Ltd. All rights reserved.
机译:Tachykinins是一系列Proticpeptive神经肽,在疼痛和炎症中具有特异性作用。几种机制调节内源性曲丘素和物质p(sp)水平,包括protachykin mRNA的差异表达和来自神经元的肠肽的分泌物。怀疑蛋白水解以调节细胞外SP浓度,但在易化肽和神经肽的代谢上进行了很少的研究。在这里,我们提供了蛋白水解控制脊髓中SP水平,导致形成有源C末端片段。使用高分辨率质谱,特征和量化特异性的曲丘素片段。 Beta-Tachykinin(58-71)和SP的代谢稳定性非常短,导致半衰期分别为5.7和3.5分钟。鉴定了几种C末端片段,包括SP3-11,SP5-11和SP8-11,其保护对神经蛋白1受体的亲和力。有趣的是,C末端片段的代谢稳定性显着优越。使用两种特异性脯氨酰内肽酶抑制剂,并显示出SP3-11和SP5-11的形成速率显着降低,提供了强大的证据,即脯氨酰内肽酶参与脊髓中SP的N-末端加工。 (c)2016 Elsevier Ltd.保留所有权利。

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