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心血管药物美速酮和坎利酮的生物转化

Biotransformations of the cardiovascular drugs mexrenone and canrenone.

作者信息

Preisig Carol L, Laakso Jodi A, Mocek Ursula M, Wang Ping T, Baez Julio, Byng Graham

机构信息

MDS Pharma Services, 11804 North Creek Parkway South, Bothell, Washington 98011, USA.

出版信息

J Nat Prod. 2003 Mar;66(3):350-6. doi: 10.1021/np020347a.

Abstract

Microbial transformation studies of the cardiovascular drugs mexrenone (1) and canrenone (2) were conducted. Thirty-nine biotransformations of mexrenone and 84 biotransformations of canrenone were analyzed. Metabolism of the substrate was observed in the majority of these cases. Several monohydroxylated derivatives were detected by HPLC-MS-UV and subsequently identified. Two new mexrenone derivatives, 11alpha- (3) and 12beta-hydroxymexrenone (4), and the known metabolite 6beta-hydroxymexrenone (5) were isolated as major products produced by the Beauveria bassiana ATCC 13144 bioconversion (3) and the Mortierella isabellina bioconversion (4 and 5), respectively. Single-elimination products were also sought; however, only the production of the known metabolite Delta(1,2)-mexrenone (6) by several bacteria was confirmed. One new monohydroxylated derivative of canrenone, 9alpha-hydroxycanrenone (7), was isolated as a major product from the Corynespora cassiicola bioconversion. Structure elucidation of all metabolites was based on NMR and HRMS analyses.

摘要

开展了心血管药物美替诺龙(1)和坎利酮(2)的微生物转化研究。分析了美替诺龙的39种生物转化产物和坎利酮的84种生物转化产物。在大多数情况下观察到了底物的代谢情况。通过高效液相色谱-质谱-紫外联用仪检测到了几种单羟基化衍生物,并随后进行了鉴定。两种新的美替诺龙衍生物,11α-(3)和12β-羟基美替诺龙(4),以及已知代谢产物6β-羟基美替诺龙(5),分别作为球孢白僵菌ATCC 13144生物转化产生的主要产物(3)和深黄被孢霉生物转化产生的主要产物(4和5)被分离出来。还寻找了单消除产物;然而,仅证实了几种细菌产生已知代谢产物Δ(1,2)-美替诺龙(6)。一种新的坎利酮单羟基化衍生物,9α-羟基坎利酮(7),作为主要产物从瓜亡革菌生物转化中分离出来。所有代谢产物的结构鉴定均基于核磁共振和高分辨质谱分析。

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