抗肿瘤卤代单萜类化合物卤霉素在小鼠和人肝脏制剂中的体外代谢

In vitro metabolism by mouse and human liver preparations of halomon, an antitumor halogenated monoterpene.

作者信息

Egorin M J, Rosen D M, Benjamin S E, Callery P S, Sentz D L, Eiseman J L

机构信息

Division of Developmental Therapeutics, University of Maryland Cancer Center, Baltimore 21201, USA.

出版信息

Cancer Chemother Pharmacol. 1997;41(1):9-14. doi: 10.1007/s002800050701.

DOI:10.1007/s002800050701

PMID:9443608

Abstract

OBJECTIVES

To characterize the enzymes responsible for and metabolites produced from the metabolism of halomon, a halogenated monoterpene that is isolated from the red algae Portieria hornemanii and has in vitro activity in the NCI screen against brain, renal, and colon cancer cell lines.

MATERIALS AND METHODS

Mouse and human liver fractions, prepared by homogenization and differential centrifugation, were incubated with halomon, extracted with toluene, and analyzed by gas chromatography.

RESULTS

In the presence of NADPH, mouse-liver 9,000-g supernatant (S9) fractions metabolized halomon, but boiled S9 fractions did not. NADH could not substitute for NADPH. Further separation of murine hepatic S9 fractions produced a microsomal fraction that contained all of the halomon-metabolizing activity; cytosol had none. Carbon monoxide reduced murine hepatic microsomal metabolism of halomon, whereas an anaerobic, N2 environment greatly accelerated the disappearance of halomon. Human hepatic microsomes metabolized halomon and required NADPH to do so. Carbon monoxide completely inhibited human hepatic microsomal metabolism of halomon. Unlike murine hepatic microsomal metabolism of halomon, anaerobic conditions did not enhance the metabolism of halomon by human hepatic microsomes. Neither 100 microM diethyldithiocarbamate, 1 microM quinidine, 100 microM ciprofloxacin, 3 microM ketoconazole, nor 100 microM sulfinpyrazone inhibited the metabolism of halomon by human hepatic microsomes. Both murine and human hepatic microsomes produced a metabolite of halomon. The mass spectrum of this metabolite indicated the loss of one chlorine atom and one bromine atom.

CONCLUSIONS

Halomon is metabolized by mouse and human hepatic cytochrome P-450 enzymes, the identities of which remain unknown. Hepatic metabolism of halomon is very consistent with the concentrations of halomon measured in mouse tissues and urine after i.v. administration of the drug.

摘要

目的

表征负责代谢卤代单萜卤霉素的酶及其代谢产物。卤霉素是从红藻霍氏波蒂埃藻中分离出的一种卤代单萜，在国立癌症研究所针对脑、肾和结肠癌细胞系的筛选中具有体外活性。

材料与方法

通过匀浆和差速离心制备的小鼠和人肝脏组分与卤霉素一起孵育，用甲苯萃取，并通过气相色谱分析。

结果

在存在烟酰胺腺嘌呤二核苷酸磷酸（NADPH）的情况下，小鼠肝脏9000克上清液（S9）组分可代谢卤霉素，但煮沸的S9组分则不能。烟酰胺腺嘌呤二核苷酸（NADH）不能替代NADPH。对小鼠肝脏S9组分进一步分离得到一个微粒体组分，其含有所有卤霉素代谢活性；胞质溶胶则无此活性。一氧化碳可降低小鼠肝脏微粒体对卤霉素的代谢，而厌氧的氮气环境则极大地加速了卤霉素的消失。人肝脏微粒体可代谢卤霉素，且需要NADPH才能进行代谢。一氧化碳完全抑制人肝脏微粒体对卤霉素的代谢。与小鼠肝脏微粒体对卤霉素的代谢不同，厌氧条件不会增强人肝脏微粒体对卤霉素的代谢。100微摩尔/升二乙基二硫代氨基甲酸盐、1微摩尔/升奎尼丁、100微摩尔/升环丙沙星、3微摩尔/升酮康唑或100微摩尔/升磺吡酮均未抑制人肝脏微粒体对卤霉素的代谢。小鼠和人肝脏微粒体均产生卤霉素的一种代谢产物。该代谢产物的质谱表明损失了一个氯原子和一个溴原子。