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使用高分辨率四极杆-轨道阱质谱法对大鼠脊髓S9组分中神经肽K的加工过程进行表征。

Characterization of neuropeptide K processing in rat spinal cord S9 fractions using high-resolution quadrupole-Orbitrap mass spectrometry.

作者信息

Salem Jennifer Ben, Nkambeu Bruno, Beaudry Francis

机构信息

Groupe de Recherche en Pharmacologie Animal du Québec, Département de Biomédecine Vétérinaire, Faculté de Médecine Vétérinaire, Université de Montréal, Québec, Canada.

出版信息

Biomed Chromatogr. 2018 Jun;32(6):e4204. doi: 10.1002/bmc.4204. Epub 2018 Feb 27.

DOI:10.1002/bmc.4204
PMID:29442375
Abstract

Tachykinins are a family of pronociceptive neuropeptides with a specific role in pain and inflammation. Several mechanisms regulate endogenous tachykinins levels, including the differential expression of protachykinin mRNA and the controlled secretion of tachykinin peptides from neurons. We suspect that proteolysis regulates extracellular neuropeptide K (NPK) and neurokinin A (NKA) concentrations and NPK is a precursor of NKA. Here, we provide evidence that proteolysis controls NPK and NKA levels in the spinal cord, leading to the formation of active C-terminal peptide fragments. Using high-resolution mass spectrometry, specific tachykinin fragments were identified and characterized. The metabolic stability in rat spinal cord fractions of NPK and NKA was very short, resulting in half-lives of 1.9 and 2.2 min respectively. Following the degradation of NPK, several C-terminal fragments were identified, including NPK , NKA, NKA , NKA , NKA and NKA , which conserve affinity for the neurokinin 2 receptor but also for the neurokinin 1 receptor. Interestingly, the same fragments were identified following the degradation of NKA. A specific proprotein convertases inhibitor was used and showed a significant reduction in the rate of formation of NKA, providing strong evidence that proprotein convertase is involved in C-terminal processing of NPK in the spinal cord, leading to the formation of NKA.

摘要

速激肽是一类在前瞻性伤害感受中起特定作用的神经肽,在疼痛和炎症反应中发挥作用。多种机制可调节内源性速激肽水平,包括前速激肽原mRNA的差异表达以及神经元中速激肽肽段的可控分泌。我们推测蛋白水解作用可调节细胞外神经肽K(NPK)和神经激肽A(NKA)的浓度,且NPK是NKA的前体。在此,我们提供证据表明蛋白水解作用可控制脊髓中NPK和NKA的水平,从而导致活性C末端肽片段的形成。通过高分辨率质谱法,鉴定并表征了特定的速激肽片段。NPK和NKA在大鼠脊髓组分中的代谢稳定性非常短,其半衰期分别为1.9分钟和2.2分钟。NPK降解后,鉴定出了几个C末端片段,包括NPK 、NKA、NKA 、NKA 、NKA和NKA ,这些片段不仅对神经激肽2受体具有亲和力,对神经激肽1受体也有亲和力。有趣的是,NKA降解后也鉴定出了相同的片段。使用了一种特异性前体蛋白转化酶抑制剂,结果显示NKA的形成速率显著降低,这有力地证明了前体蛋白转化酶参与了脊髓中NPK的C末端加工过程,从而导致NKA的形成。

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Multiple molecular forms of tachykinins in rat spinal cord: a study comparing different extraction methods.大鼠脊髓中速激肽的多种分子形式:比较不同提取方法的研究
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