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哺乳动物组织中膜结合型氨基脲敏感胺氧化酶(SSAO)活性的选择性抑制剂。

Selective inhibitors of membrane-bound semicarbazide-sensitive amine oxidase (SSAO) activity in mammalian tissues.

作者信息

Kinemuchi Hiroyasu, Sugimoto Haruyo, Obata Toshio, Satoh Nobunori, Ueda Shiro

机构信息

Laboratory of Enzyme Pharmacology, Senshu University at Ishinomaki, Ishinomaki 986-8580, Japan.

出版信息

Neurotoxicology. 2004 Jan;25(1-2):325-35. doi: 10.1016/S0161-813X(03)00118-9.

Abstract

Semicarbazide-sensitive amine oxidase (SSAO, EC 1.4.3.6) is a group of enzymes highly sensitive to inhibition by semicarbazide. This high sensitivity distinguishes these enzymes from monoamine oxidase (MAO). Various mammalian tissues contain membrane-bound SSAO which metabolizes only the primary monoamines. Vascular and non-vascular smooth muscle cells have particularly high SSAO activity, but recently the enzyme activity has also been found in non-vascular smooth muscle cells. The substrate specificity of SSAO shows considerable species-related variations. A variety of compounds inhibiting MAO activity has also been identified as SSAO inhibitors. Among inhibitors, there is no specific SSAO inhibitor so far tested. Many studies reinforce the conclusion that inhibitory properties of some compounds against MAO activities has been markedly differed from their properties as SSAO inhibitors. 2-bromoethylamine has been recently developed with a potent, selective and suicide SSAO inhibitor without any inhibitory effect on MAO activity Using this inhibitor, it is possible to study the role of the enzyme in mammalian tissues. As physiological role the increased concentrations of SSAO, especially in blood plasma, have been found in diabetic patients and experimental animals. This enzyme was found to be associated with translocation of the glucose transporter GLUT 4 into the adipose cell surface and involved in the signaling of glucose uptake. Recent studies showed that vascular SSAO metabolizes endogenous primary amines, allylamine, methylamine and aminoacetone, to the corresponding cytotoxic aldehydes. These aldehydes have been linked to the ability of diabetic complications such as neuropathy, retinopathy and nephropathy. Overproduction of such toxic aldehydes produced by increased SSAO activity was proposed to be potentially hazardous in diabetic complications. Thus, reduction or inhibition of SSAO may be beneficial in these pathological conditions. Clearly species-related differences in properties of SSAO must be taken into account in this respect, particularly when assessing if SSAO inhibition may have great application in human.

摘要

氨基脲敏感胺氧化酶(SSAO,EC 1.4.3.6)是一类对氨基脲抑制作用高度敏感的酶。这种高敏感性使这些酶与单胺氧化酶(MAO)区分开来。各种哺乳动物组织都含有膜结合的SSAO,它只代谢伯单胺。血管和平滑肌细胞具有特别高的SSAO活性,但最近在非血管平滑肌细胞中也发现了该酶活性。SSAO的底物特异性表现出相当大的物种相关差异。多种抑制MAO活性的化合物也被鉴定为SSAO抑制剂。在抑制剂中,目前还没有经过测试的特异性SSAO抑制剂。许多研究强化了这样的结论,即一些化合物对MAO活性的抑制特性与它们作为SSAO抑制剂的特性明显不同。2-溴乙胺最近被开发为一种强效、选择性和自杀性的SSAO抑制剂,对MAO活性没有任何抑制作用。使用这种抑制剂,可以研究该酶在哺乳动物组织中的作用。作为生理作用,在糖尿病患者和实验动物中发现SSAO浓度升高,尤其是在血浆中。发现这种酶与葡萄糖转运蛋白GLUT 4向脂肪细胞表面的转位有关,并参与葡萄糖摄取的信号传导。最近的研究表明,血管SSAO将内源性伯胺、烯丙胺、甲胺和氨基丙酮代谢为相应的细胞毒性醛。这些醛与糖尿病并发症如神经病变、视网膜病变和肾病的发生能力有关。有人提出,SSAO活性增加产生的这种有毒醛的过量产生在糖尿病并发症中可能具有潜在危害。因此,降低或抑制SSAO在这些病理状况下可能是有益的。在这方面,必须考虑到SSAO特性明显的物种相关差异,特别是在评估SSAO抑制是否可能在人类中有广泛应用时。

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