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大鼠输精管中氨基脲敏感胺氧化酶(SSAO)对多巴胺的氧化作用。

The oxidation of dopamine by the semicarbazide-sensitive amine oxidase (SSAO) from rat vas deferens.

作者信息

Lizcano J M, Balsa D, Tipton K F, Unzeta M

机构信息

Departament de Bioquímica i Biologia Molecular, Facultat de Medicina, Universitat Autonoma de Barcelona, Spain.

出版信息

Biochem Pharmacol. 1991 Apr 15;41(8):1107-10. doi: 10.1016/0006-2952(91)90647-n.

Abstract

The activities of monoamine oxidase A and B and the semicarbazide-sensitive amine oxidase from rat vas deferens were compared towards benzylamine and dopamine. The selective inhibitors (-)-deprenyl and clorgyline were used to allow the contributions of the A and B forms of monoamine oxidase to be determined separately. Comparison of the kinetic constants of the three enzymes towards dopamine indicated that, although each of them had activity towards this substrate, their relative contributions to the total oxidative deamination would depend on the substrate concentration. At all concentrations in the range 1 microM to 10 mM monoamine oxidase-B would contribute about 50% of the total activity. In the range 1 to 10 microM the contributions made by activities of monoamine oxidase-A and the semicarbazide-sensitive enzyme were similar but at higher concentrations the activity of the latter enzyme became more important, its contribution to the total activity rising to some 35% of the total at 500 microM dopamine. The activity of the semicarbazide-sensitive enzyme towards dopamine might thus be important under conditions where either or both the monoamine oxidases were inhibited in pharmacological studies. Its possible relevance to Norrie disease, in which both forms of the human enzyme are deficient, requires further examination.

摘要

比较了大鼠输精管中A、B型单胺氧化酶和氨基脲敏感胺氧化酶对苄胺和多巴胺的活性。使用选择性抑制剂(-)-司来吉兰和氯吉兰来分别确定单胺氧化酶A和B型的作用。三种酶对多巴胺的动力学常数比较表明,尽管它们都对该底物有活性,但其对总氧化脱氨基作用的相对贡献将取决于底物浓度。在1微摩尔至10毫摩尔范围内的所有浓度下,单胺氧化酶B对总活性的贡献约为50%。在1至10微摩尔范围内,单胺氧化酶A和氨基脲敏感酶的活性贡献相似,但在较高浓度下,后一种酶的活性变得更为重要,在500微摩尔多巴胺时,其对总活性的贡献上升至约35%。因此,在药理学研究中,当单胺氧化酶中的一种或两种被抑制时,氨基脲敏感酶对多巴胺的活性可能很重要。其与诺里病(人类该酶的两种形式均缺乏)的可能相关性需要进一步研究。

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