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首页> 外文期刊>Japanese Journal of Pharmacology >FURTHER STUDIES ON THE SYNTHESIS OF A-FORM MONOAMINE OXIDASE
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FURTHER STUDIES ON THE SYNTHESIS OF A-FORM MONOAMINE OXIDASE

机译:进一步研究合成α-单胺氧化酶

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References(19) Cited-By(13) The relation between precursors and restoration of A-form MAO activity in rat liver after administration of clorgyline to rats was investigated by measuring the rates of recovery of A-form MAO activity after treatment with the inhibitor. The half-lives of mitochondrial and microsomal A-form MAO were estimated as 3.5 and 2.0 days, respectively. MAO activity and the amount of MAO molecules were completely restored within 14 days. However the values attained did not exceed the control values in a period of 14 days. Clorgyline plus cycloheximide or chloramphenicol did not prevent the recovery of MAO activity in the microsomes, but did not delay the appearance of enzyme activity in the mitochondria. A and B-form-like MAO were also observed in the microsomal and supernatant fractions, with clorgyline as inhibitor. These results suggest that the microsomal enzyme is a precursor of the mitochondrial enzyme, that the levels of A-form and B-form MAO are regulated genetically, and that the two forms of MAO may be synthesized separately.
机译:参考文献(19)引用(13)通过测量用抑制剂治疗后α-型MAO活性的回收率进行研究前体前体与大鼠肝脏恢复的α-型MAO活性的关系。 。线粒体和微粒体A形MAO的半衰期分别估计为3.5和2.0天。 Mao活动和MAO分子的数量在14天内完全恢复。然而,达到的值在14天内没有超过控制值。 Clorgyline Plus环己酰亚胺或氯霉素没有防止在微粒体中恢复MAO活性,但未延迟线粒体中酶活性的外观。在微粒体和上清液级分中也观察到A和B形状的MAO,用Clorgyline作为抑制剂。这些结果表明,微粒体酶是线粒体酶的前体,即遗传调节A形和B形MAO的水平,并且可以单独合成两种形式的MAO。

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