首页> 外文期刊>Biochimica et biophysica acta. Molecular basis of disease: BBA >Activation of human lung semicarbazide sensitive amine oxidase by a low molecular weight component present in human plasma
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Activation of human lung semicarbazide sensitive amine oxidase by a low molecular weight component present in human plasma

机译:人血浆中存在的低分子量组分激活人肺氨基脲化合物敏感的胺氧化酶

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Semicarbazide-sensitive amine oxidase (SSAO) encodes a wide family of enzymes named E. C. 1.4.3.6 [maine: oxygen oxidoreductase (deaminating)(copper containing)] that metabolises primary aliphatic and aromatic amines. It is present in almost all vascularised and nonvascularised mammalian tissues, and it is also present in soluble form in plasma. SSAO appears to show different functions depending on th tissue where it is expressed. Here we describe, for the first time, the activation of the SSAO from human lung by human plasma. The extent of activation was greater when the human plasma came from diabetic and heart infarcted patients. A kinetic mechanism of such effect is proposed. The activation was lost after the plasma was dialysed, indicating a low molecular weight component (MW < 3800 Da) to be responsible. The activator component is heat stable and resistant to proteolysis by chymotrypsin and trypsin and also resistant to perchloric acid treatment. However, treatment with 35% formic acid, completely abolished activation, suggesting involvement of lipid material. The possibility of that lysophosphatidylcholine (LPC), an amphiphilic phospholipid derived from the phosphatidylcholine, the major component in plasma accumulated in pathological conditions, was studied. LPC was shown the behave as a "competitive activator" of human lung SSAO at concentrations below its critical micellar concentration (CMC value = 50 μM). Thus LPC may be a component of the SSAO activatory material present in human plasma.
机译:氨基脲敏感的胺氧化酶(SSAO)编码一系列广泛的酶,称为E. C. 1.4.3.6 [maine:氧氧化还原酶(脱氨)(含铜)],可代谢脂肪族和芳香族伯胺。它几乎存在于所有血管化和非血管化的哺乳动物组织中,并且也以可溶形式存在于血浆中。 SSAO似乎表现出不同的功能,具体取决于表达它的组织。在这里,我们首次描述了人血浆从人肺激活SSAO的过程。当人血浆来自糖尿病和心脏梗塞患者时,激活程度更大。提出了这种作用的动力学机理。透析血浆后失去激活,表明是低分子量组分(MW <3800 Da)。活化剂组分是热稳定的,并且对胰凝乳蛋白酶和胰蛋白酶的蛋白水解具有抵抗力,并且还对高氯酸处理具有抵抗力。但是,用35%甲酸处理完全取消了活化作用,表明脂质物质参与其中。研究了溶血磷脂酰胆碱(LPC)(一种衍生自磷脂酰胆碱的两亲性磷脂)的可能性,磷脂酰胆碱是病理条件下血浆中的主要成分。在低于其临界胶束浓度(CMC值= 50μM)的浓度下,LPC表现为人肺SSAO的“竞争性激活剂”。因此,LPC可能是人血浆中存在的SSAO活化材料的成分。

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