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辅因子和物种差异对苯丙酮和苯乙酮体外代谢的影响。

The effects of cofactor and species differences on the in vitro metabolism of propiophenone and phenylacetone.

作者信息

Coutts R T, Prelusky D B, Jones G R

出版信息

Can J Physiol Pharmacol. 1981 Feb;59(2):195-201. doi: 10.1139/y81-032.

Abstract

In vitro metabolism of the aromatic ketone propiophenone and its nonaromatic isomer phenylacetone was studied using fortified 12 000 X g supernatants of liver homogenates from rat and rabbit. Reduction to the corresponding alcohols was the major metabolic route observed, although aliphatic C-hydroxylation and alcohol dehydrogenation also occurred. Marked differences were observed in the amounts of carbonyl reduction of the substrates, which was dependent on the species as well as the cofactor employed. Using rat liver preparation, phenylacetone was reduced to 1-phenyl-2-propanol much more efficiently with an NADH-fortified system than when NADPH was used whereas in rabbit, extensive reduction occurred in the presence of either cofactor. Reduction of propiophenone to 1-phenyl-1-propanol by rat liver preparation was slightly greater in the presence of NADH than with NADPH; the converse was observed in rabbit. Aliphatic hydroxylation of propiophenone to 2-hydroxy-1-phenyl-1-propanone was also a significant metabolic pathway in both species, with NADPH being the more efficient cofactor, but C-1 hydroxylation of phenylacetone to 1-hydroxy-1-phenyl-2-propanone occurred only to a minor extent. Small amounts of 1-phenyl-1,2-propanedione, as well as both erythro and threo isomers of 1-phenyl-1,2-propanediol, were also identified as metabolites in both species. Similar metabolic studies were carried out on the alcohols 1-phenyl-1-propanol and 1-phenyl-2-propanol and again the nature and quantities of metabolites isolated showed both species and cofactor dependencies.

摘要

使用大鼠和家兔肝脏匀浆经12000×g离心后的强化上清液,对芳香酮苯丙酮及其非芳香异构体苯乙酮的体外代谢进行了研究。尽管也发生了脂肪族碳羟基化和醇脱氢反应,但还原为相应的醇是观察到的主要代谢途径。在底物羰基还原量方面观察到显著差异,这取决于物种以及所使用的辅因子。使用大鼠肝脏制剂时,在NADH强化系统中,苯乙酮还原为1-苯基-2-丙醇的效率比使用NADPH时要高得多;而在家兔中,在任何一种辅因子存在下都发生了广泛的还原反应。大鼠肝脏制剂将苯丙酮还原为1-苯基-1-丙醇,在NADH存在下比在NADPH存在下略多;在家兔中观察到相反的情况。苯丙酮脂肪族羟基化生成2-羟基-1-苯基-1-丙醇在两个物种中也是一条重要的代谢途径,NADPH是更有效的辅因子,但苯乙酮C-1羟基化生成1-羟基-1-苯基-2-丙醇的程度较小。在两个物种中还鉴定出少量的1-苯基-1,2-丙二酮以及1-苯基-1,2-丙二醇的赤藓糖和苏阿糖异构体作为代谢产物。对醇类1-苯基-1-丙醇和1-苯基-2-丙醇进行了类似的代谢研究,分离得到的代谢产物的性质和数量同样显示出对物种和辅因子的依赖性。

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