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氯丙嗪对肝脏、大脑和小脑中黄素代谢的甲状腺素调节作用的抑制。

Inhibition by chlorpromazine of thyroxine modulation of flavin metabolism in liver, cerebrum and cerebellum.

作者信息

Pinto J, Huang Y P, Rivlin R S

出版信息

Biochem Pharmacol. 1985 Jan 1;34(1):93-5. doi: 10.1016/0006-2952(85)90105-4.

Abstract

In livers of adult rats that have been treated with thyroxine, the rate of incorporation of radiolabeled riboflavin into both flavin adenine dinucleotide (FAD) and FAD covalently attached to specific apoflavoenzymes was enhanced markedly. By contrast, thyroxine diminished riboflavin incorporation into FAD in cerebrum and cerebellum but continued to enhance incorporation into the covalently bound fraction of FAD. Diminished net incorporation of riboflavin into FAD in brains of adult rats may reflect increased utilization of this fraction for covalent attachment into specific apoflavoenzymes rather than down regulation of the FAD biosynthetic enzymes, flavokinase and FAD pyrophosphorylase, inasmuch as covalent attachment of FAD occurs subsequent to the formation of FAD. The psychotropic drug, chlorpromazine, over a wide dose range, exerted an inhibitory effect on both incorporation of riboflavin into FAD and the utilization of FAD for incorporation into covalently bound flavoenzymes in liver, cerebrum, and cerebellum. Thus, chlorpromazine inhibition of FAD metabolism occurred regardless of the direction of the thyroxine effect and was compatible with an observed inhibitory effect by this drug upon the flavin biosynthetic enzymes.

摘要

在经甲状腺素处理的成年大鼠肝脏中,放射性标记核黄素掺入黄素腺嘌呤二核苷酸(FAD)以及与特定脱辅基黄素酶共价结合的FAD中的速率均显著提高。相比之下,甲状腺素减少了核黄素在大脑和小脑中掺入FAD的量,但继续提高其掺入FAD共价结合部分的量。成年大鼠大脑中核黄素净掺入FAD量的减少可能反映出该部分用于共价结合到特定脱辅基黄素酶的利用率增加,而非FAD生物合成酶(黄素激酶和FAD焦磷酸化酶)的下调,因为FAD的共价结合发生在FAD形成之后。精神药物氯丙嗪在很宽的剂量范围内,对肝脏、大脑和小脑中核黄素掺入FAD以及FAD用于掺入共价结合黄素酶的利用率均产生抑制作用。因此,无论甲状腺素作用的方向如何,氯丙嗪均抑制FAD代谢,且这与该药物对黄素生物合成酶的抑制作用相符。

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