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糖尿病患者肝脏中细胞色素 P450 3A4 的表达和活性显著降低。

Significantly reduced cytochrome P450 3A4 expression and activity in liver from humans with diabetes mellitus.

机构信息

Department of Biomedical and Pharmaceutical Sciences, University of Rhode Island, Kingston, RI, USA.

出版信息

Br J Pharmacol. 2011 Jul;163(5):937-47. doi: 10.1111/j.1476-5381.2011.01270.x.

Abstract

BACKGROUND AND PURPOSE

Patients with diabetes mellitus require pharmacotherapy with numerous medications. However, the effect of diabetes on drug biotransformation is not well understood. Our goal was to investigate the effect of diabetes on liver cytochrome P450 3As, the most abundant phase I drug-metabolizing enzymes in humans.

EXPERIMENTAL APPROACH

Human liver microsomal fractions (HLMs) were prepared from diabetic (n= 12) and demographically matched nondiabetic (n= 12) donors, genotyped for CYP3A41B and CYP3A53 polymorphisms. Cytochrome P450 3A4, 3A5 and 2E1 mRNA expression, protein level and enzymatic activity were compared between the two groups.

KEY RESULTS

Midazolam 1'- or 4-hydroxylation and testosterone 6β-hydroxylation, catalyzed by P450 3A, were markedly reduced in diabetic HLMs, irrespective of genotype. Significantly lower P450 3A4 protein and comparable mRNA levels were observed in diabetic HLMs. In contrast, neither P450 3A5 protein level nor mRNA expression differed significantly between the two groups. Concurrently, we have observed increased P450 2E1 protein level and higher chlorzoxazone 6-hydroxylation activity in diabetic HLMs.

CONCLUSIONS AND IMPLICATIONS

These studies indicate that diabetes is associated with a significant decrease in hepatic P450 3A4 enzymatic activity and protein level. This finding could be clinically relevant for diabetic patients who have additional comorbidities and are receiving multiple medications. To further characterize the effect of diabetes on P450 3A4 activity, a well-controlled clinical study in diabetic patients is warranted.

摘要

背景与目的

糖尿病患者需要使用多种药物进行药物治疗。然而,糖尿病对药物生物转化的影响尚不清楚。我们的目标是研究糖尿病对人类中最丰富的 I 相药物代谢酶肝细胞色素 P450 3A 的影响。

实验方法

从糖尿病(n=12)和年龄匹配的非糖尿病(n=12)供体中制备人肝微粒体部分(HLM),并对 CYP3A41B 和 CYP3A53 多态性进行基因分型。比较两组之间细胞色素 P450 3A4、3A5 和 2E1 mRNA 表达、蛋白水平和酶活性。

主要结果

咪达唑仑 1'-或 4-羟化和睾酮 6β-羟化,由 P450 3A 催化,在糖尿病 HLMs 中显著降低,与基因型无关。在糖尿病 HLMs 中观察到显著较低的 P450 3A4 蛋白和可比的 mRNA 水平。相比之下,两组之间 P450 3A5 蛋白水平或 mRNA 表达没有显著差异。同时,我们观察到糖尿病 HLMs 中 P450 2E1 蛋白水平升高和氯唑沙宗 6-羟化活性升高。

结论和意义

这些研究表明,糖尿病与肝 P450 3A 酶活性和蛋白水平显著降低有关。对于患有其他合并症并接受多种药物治疗的糖尿病患者,这一发现可能具有临床相关性。为了进一步描述糖尿病对 P450 3A4 活性的影响,需要在糖尿病患者中进行一项精心控制的临床研究。

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