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他汀类药物的耐受性与细胞色素P450(CYP450)基因多态性无关,但细胞色素P2D6(CYP2D6)代谢的降低可改善辛伐他汀和氟伐他汀的降胆固醇反应。

Tolerability of statins is not linked to CYP450 polymorphisms, but reduced CYP2D6 metabolism improves cholesteraemic response to simvastatin and fluvastatin.

作者信息

Zuccaro Piergiorgio, Mombelli Giuliana, Calabresi Laura, Baldassarre Damiano, Palmi Ilaria, Sirtori Cesare R

机构信息

Department of Drug Research and Evaluation, Italian National Institute of Health, Rome, Italy.

出版信息

Pharmacol Res. 2007 Apr;55(4):310-7. doi: 10.1016/j.phrs.2006.12.009. Epub 2007 Jan 14.

Abstract

Statin therapy, although generally well tolerated, leads not infrequently to significant subjective and at times objective adverse effects (AEs), mainly of a muscular nature. The genetic background of these AEs is not clear and possibly side effects and lipid lowering efficacy may be linked. Aim of the study was a detailed evaluation of CYP450 and apolipoprotein E gene polymorphisms in two large series of age-sex matched patients with and without muscular side effects to statins. In a Clinical Institution specialised in lipid-lipoprotein disorders, 50 statin treated patients were selected, with subjective or objective statin-associated myopathy, evaluated using standardized forms. These were sex and age matched with 50 statin-treated patients from the same Clinic, without any subjective or objective complaints. DNA samples for the evaluation of CYP450 genetic polymorphisms and apo E genotypes were collected in order to assess correlations with both genetic polymorphisms and AEs, as well as with therapeutic efficacy. None of the assessed CYP450 polymorphisms appeared to be related to an increased incidence of AEs. The CYP2D6 *1/*4 and 4/4 poor metabolizer (PM) status was associated to a higher efficacy of statins metabolized by this system and, in addition, the apo E2 genotype was, in this series, linked to increased HDL-C levels after therapy. Patients with statin associated myopathy are not characterized by significantly different genotypes for the CYP450s responsible for statin metabolism. On the other hand, CYP2D6 PM status is associated to an increased efficacy of statins metabolized by this system.

摘要

他汀类药物治疗虽然总体耐受性良好,但常常会导致显著的主观不良反应,有时还会出现客观不良反应(AE),主要是肌肉方面的。这些不良反应的遗传背景尚不清楚,副作用和降脂疗效可能存在关联。本研究的目的是详细评估两组年龄和性别匹配的服用他汀类药物且有或无肌肉副作用的患者的细胞色素P450(CYP450)和载脂蛋白E基因多态性。在一家专门治疗脂质 - 脂蛋白紊乱的临床机构中,选取了50例接受他汀类药物治疗且患有主观或客观他汀类药物相关性肌病的患者,使用标准化表格进行评估。这些患者在性别和年龄上与同一家诊所的50例接受他汀类药物治疗但无任何主观或客观不适的患者相匹配。收集用于评估CYP450基因多态性和载脂蛋白E基因型的DNA样本,以评估与基因多态性、不良反应以及治疗效果之间的相关性。所评估的CYP450多态性似乎均与不良反应发生率增加无关。CYP2D6 1/4和4/4慢代谢者(PM)状态与该系统代谢的他汀类药物更高的疗效相关,此外,在本系列研究中,载脂蛋白E2基因型与治疗后高密度脂蛋白胆固醇(HDL - C)水平升高有关。他汀类药物相关性肌病患者在负责他汀类药物代谢的CYP450基因型方面并无显著差异。另一方面,CYP2D6 PM状态与该系统代谢的他汀类药物疗效增加有关。

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