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尿中6β-羟基皮质醇排泄增加作为人类肝细胞色素P450IIIA诱导的标志物。

The increase in urinary excretion of 6 beta-hydroxycortisol as a marker of human hepatic cytochrome P450IIIA induction.

作者信息

Ged C, Rouillon J M, Pichard L, Combalbert J, Bressot N, Bories P, Michel H, Beaune P, Maurel P

机构信息

INSERM U 75, Hôpital Necker-Enfants Malades, Paris, France.

出版信息

Br J Clin Pharmacol. 1989 Oct;28(4):373-87. doi: 10.1111/j.1365-2125.1989.tb03516.x.

Abstract
  1. Urinary excretion of 6 beta-hydroxycortisol, hepatic microsomal cortisol 6 beta-hydroxylase and the specific content of several forms of cytochrome P450 were measured in 8 to 14 patients before and after treatment with rifampicin (600 mg orally per day for 4 days). 2. Rifampicin treatment produced an average five fold increase in daily excretion of urinary 6 beta-hydroxycortisol. 3. Cortisol 6 beta-hydroxylase activity increased from 15 +/- 6 pmol min-1 mg-1 in organ donors (considered as 'control subjects') to 87 +/- 31 pmol min-1 mg-1 in rifampicin treated patients. 4. Among three forms of human P450 (P450IA, IIC and IIIA), (1), (2), measured by Western blots, only P450IIIA was significantly induced by the antibiotic. 5. Only antibodies against P450IIIA selectively inhibited cortisol 6 beta-hydroxylase in human liver microsomes. 6. Cortisol 6 beta-hydroxylase was correlated with P450IIIA specific content. 7. The urinary level of 6 beta-hydroxycortisol correlated with liver microsomal cortisol 6 beta-hydroxylase and P450IIIA specific content. 8. We conclude that P450IIIA is predominantly responsible for cortisol 6 beta-hydroxylase activity in human liver microsomes and that urinary 6 beta-hydroxycortisol is a marker of the induction of this cytochrome P450.
摘要
  1. 对8至14名患者在使用利福平治疗前后(每天口服600毫克,共4天),测量了6β-羟基皮质醇的尿排泄量、肝微粒体皮质醇6β-羟化酶以及几种细胞色素P450形式的比含量。2. 利福平治疗使尿中6β-羟基皮质醇的每日排泄量平均增加了五倍。3. 皮质醇6β-羟化酶活性从器官捐献者(视为“对照受试者”)的15±6皮摩尔·分钟⁻¹·毫克⁻¹增加到利福平治疗患者的87±31皮摩尔·分钟⁻¹·毫克⁻¹。4. 在通过蛋白质印迹法测量的三种人类P450(P450IA、IIC和IIIA)形式中,只有P450IIIA被该抗生素显著诱导。5. 只有针对P450IIIA的抗体选择性地抑制人肝微粒体中的皮质醇6β-羟化酶。6. 皮质醇6β-羟化酶与P450IIIA比含量相关。7. 6β-羟基皮质醇的尿水平与肝微粒体皮质醇6β-羟化酶和P450IIIA比含量相关。8. 我们得出结论,P450IIIA在人肝微粒体中主要负责皮质醇6β-羟化酶活性,并且尿中6β-羟基皮质醇是这种细胞色素P450诱导的标志物。
https://cdn.ncbi.nlm.nih.gov/pmc/blobs/bbce/1379986/3c8a5030bf42/brjclinpharm00080-0015-a.jpg

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