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Kinetic Study of Neuropeptide Y (NPY) Proteolysis in Blood and Identification of NPY3–35

机译:血液中神经肽Y(NPY)蛋白水解的动力学研究和NPY3–35的鉴定

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摘要

There is little information on how neuropeptide Y (NPY) proteolysis by peptidases occurs in serum, in part because reliable techniques are lacking to distinguish different NPY immunoreactive forms and also because the factors affecting the expression of these enzymes have been poorly studied. In the present study, LC-MS/MS was used to identify and quantify NPY fragments resulting from peptidolytic cleavage of NPY1–36 upon incubation with human serum. Kinetic studies indicated that NPY1–36 is rapidly cleaved in serum into 3 main fragments with the following order of efficacy: NPY3–36 ≫ NPY3–35 > NPY2–36. Trace amounts of additional NPY forms were identified by accurate mass spectrometry. Specific inhibitors of dipeptidyl peptidase IV, kallikrein, and aminopeptidase P prevented the production of NPY3–36, NPY3–35, and NPY2–36, respectively. Plasma kallikrein at physiological concentrations converted NPY3–36 into NPY3–35. Receptor binding assays revealed that NPY3–35 is unable to bind to NPY Y1, Y2, and Y5 receptors; thus NPY3–35 may represent the major metabolic clearance product of the Y2/Y5 agonist, NPY3–36.
机译:关于肽酶如何在血清中发生神经肽Y(NPY)蛋白质水解的信息很少,部分原因是缺乏可靠的技术来区分不同的NPY免疫反应形式,并且因为影响这些酶表达的因素研究不足。在本研究中,LC-MS / MS用于鉴定和定量与人血清孵育后肽水解裂解NPY1-36产生的NPY片段。动力学研究表明,NPY1-36在血清中迅速裂解为3个主要片段,其效力顺序如下:NPY3-36 36 NPY3-35> NPY2-36。通过准确的质谱鉴定了痕量的其他NPY形式。二肽基肽酶IV,激肽释放酶和氨基肽酶P的特定抑制剂分别阻止了NPY3–36,NPY3–35和NPY2–36的产生。血浆激肽释放酶以生理浓度将NPY3–36转化为NPY3–35。受体结合试验表明,NPY3-35无法与NPY Y1,Y2和Y5受体结合。因此,NPY3-35可能代表Y2 / Y5激动剂NPY3-36的主要代谢清除产物。

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