贝特类药物治疗不会改变人肝脏中酰基辅酶A氧化酶的表达。

Fibrate treatment does not modify the expression of acyl coenzyme A oxidase in human liver.

作者信息

Roglans Núria, Bellido Antonia, Rodríguez Cristina, Cabrero Agatha, Novell Ferran, Ros Emilio, Zambón Daniel, Laguna Juan C

机构信息

Pharmacology Unit, Faculty of Pharmacy, University of Barcelona, Surgical Department and Lipid Clinic, Nutrition and Dietetics Service, Hospital Clínic i Provincial, Spain.

出版信息

Clin Pharmacol Ther. 2002 Dec;72(6):692-701. doi: 10.1067/mcp.2002.128605.

DOI:10.1067/mcp.2002.128605

PMID:12496750

Abstract

BACKGROUND AND OBJECTIVES

Fibrates induce hepatic peroxisome proliferation and carcinogenesis in rodents by activating peroxisome proliferator-activated receptor alpha (PPAR(alpha)). There is no conclusive evidence that humans are unresponsive to peroxisome proliferation, and concern exists about the long-term safety of fibrate treatment.

METHODS

In a university hospital setting, 48 patients with uncomplicated gallstones and a serum level of low-density lipoprotein cholesterol greater than 130 mg/dL were randomly assigned to open-label treatment with bezafibrate (400 mg/d), fenofibrate (200 mg/d), gemfibrozil (900 mg/d), or placebo for 8 weeks before elective cholecystectomy. Serum samples for lipid determinations were obtained at baseline and before surgery. A liver specimen was obtained at operation, and the relative levels of messenger ribonucleic acid (mRNA) for the wild and truncated forms of PPAR(alpha), acyl coenzyme A oxidase, liver carnitine palmitoyltransferase I, apolipoprotein A-I, and stearoyl coenzyme A desaturase were determined.

RESULTS

Fenofibrate, bezafibrate, and gemfibrozil reduced plasma low-density lipoprotein cholesterol levels by 22% (P =.009), 14% (P =.042), and 11% (not significant), respectively. Plasma triglyceride levels decreased significantly (24%-36%; P <.05), whereas high-density lipoprotein cholesterol levels rose nonsignificantly after treatment with the 3 fibrates. Except for a 35% increase of apolipoprotein A-I mRNA after fenofibrate administration (P <.05), none of the individual fibrates induced significant changes in the mRNAs tested, although as a group they increased the mRNA for liver carnitine palmitoyltransferase I by 40%(P =.08; marginally significant).

CONCLUSIONS

Fibrate administration to humans at pharmacologic doses able to activate PPAR(alpha) and to induce a hypolipidemic effect does not increase the hepatic expression of acyl coenzyme A oxidase, a well-known marker of peroxisome proliferation in rodents.

摘要

背景与目的

贝特类药物通过激活过氧化物酶体增殖物激活受体α（PPARα）诱导啮齿动物肝脏过氧化物酶体增殖和致癌。尚无确凿证据表明人类对过氧化物酶体增殖无反应，且人们对贝特类药物治疗的长期安全性存在担忧。

方法

在一所大学医院，48例单纯性胆结石且血清低密度脂蛋白胆固醇水平高于130mg/dL的患者被随机分配接受开放标签治疗，分别给予苯扎贝特（400mg/d）、非诺贝特（200mg/d）、吉非贝齐（900mg/d）或安慰剂，为期8周，然后进行择期胆囊切除术。在基线和手术前采集用于血脂测定的血清样本。手术时获取肝脏标本，测定PPARα野生型和截短型、酰基辅酶A氧化酶、肝脏肉碱棕榈酰转移酶I、载脂蛋白A-I和硬脂酰辅酶A去饱和酶的信使核糖核酸（mRNA）相对水平。

结果

非诺贝特、苯扎贝特和吉非贝齐分别使血浆低密度脂蛋白胆固醇水平降低22%（P = 0.009）、14%（P = 0.042）和11%（无统计学意义）。血浆甘油三酯水平显著降低（24% - 36%；P < 0.05），而用这三种贝特类药物治疗后高密度脂蛋白胆固醇水平无显著升高。除非诺贝特给药后载脂蛋白A-I mRNA增加35%（P < 0.05）外，尽管作为一组它们使肝脏肉碱棕榈酰转移酶I的mRNA增加了40%（P = 0.08；接近显著），但单独一种贝特类药物均未引起所检测mRNA的显著变化。