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给患有肝脏疾病的血脂异常患者开具他汀类药物处方:风险与获益之间的微妙平衡。

Prescription of statins to dyslipidemic patients affected by liver diseases: a subtle balance between risks and benefits.

作者信息

Anfossi G, Massucco P, Bonomo K, Trovati M

机构信息

Metabolic Disease and Diabetes Unit, Department of Clinical and Biological Sciences of the University of Turin, San Luigi Gonzaga Hospital, Orbassano (TO), Italy.

出版信息

Nutr Metab Cardiovasc Dis. 2004 Aug;14(4):215-24. doi: 10.1016/s0939-4753(04)80008-5.

Abstract

AIM

Statins reduce cardiovascular morbidity and mortality in the general population with an excellent risk-benefit profile. The most frequent adverse events are myopathy and increase in hepatic aminotransferases. In this review, we consider the role of liver in metabolism of statins, their potential hepatic toxicity and the guidelines for their prescription in patients affected by different liver diseases.

DATA SYNTHESIS

Statin-induced hepatic toxicity: i) occurs in 1-3% of patients; ii) is characterized by increased aminotransferase levels; iii) is dose-related; iv) is frequently asymptomatic; v) usually reverts after dosage reduction or treatment withdrawal. Finally, after recovery, a rechallenge with the same or other statins may not result in increased aminotranferases.

CONCLUSIONS

Caution is needed when prescribing statins to patients with liver disease, and liver toxicity should always be monitored during statin treatment. In particular, i) the potential hepatic toxicity requires frequent control of biochemical parameters related to hepatic cytolysis and cholestasis in all patients on statins; ii) administration of statins is counterindicated in patients with advanced or end-stage parenchymal liver disease due to the relevant impairment of their metabolism; iii) cholestatic disorders with secondary dyslipidemia do not require statin treatment even if relevant alterations of the lipid pattern are detected; iv) patients with acute liver disease of viral or alcoholic etiology should not receive statins until normalization of cytolysis enzymes; v) chronic hepatitis patients may be treated by statins if their cardiovascular risk is elevated and provided that careful follow-up is carried out to rapidly recognize the onset of further liver damage; vi) liver transplantation recipients affected by dyslipidemia induced by immunosuppressive therapy can be treated with statins under careful clinical control; vii) the benefits of statins should likely overcome the risks in the large majority of dyslipidemic patients affected by non-alcoholic hepatosteatosis, a disease frequently diagnosed in insulin-resistant subjects.

摘要

目的

他汀类药物可降低普通人群的心血管发病率和死亡率,具有良好的风险效益比。最常见的不良事件是肌病和肝转氨酶升高。在本综述中,我们探讨肝脏在他汀类药物代谢中的作用、其潜在的肝毒性以及不同肝病患者使用他汀类药物的处方指南。

资料综合

他汀类药物引起的肝毒性:i)发生在1% - 3%的患者中;ii)表现为转氨酶水平升高;iii)与剂量相关;iv)通常无症状;v)通常在减量或停药后恢复。最后,恢复后,再次使用相同或其他他汀类药物可能不会导致转氨酶升高。

结论

给肝病患者开他汀类药物时需谨慎,他汀类药物治疗期间应始终监测肝毒性。特别是,i)所有服用他汀类药物的患者,其潜在的肝毒性需要频繁控制与肝细胞溶解和胆汁淤积相关的生化参数;ii)晚期或终末期实质性肝病患者因代谢相关损害而禁忌使用他汀类药物;iii)继发性血脂异常的胆汁淤积性疾病即使检测到血脂模式有相关改变也不需要他汀类药物治疗;iv)病毒或酒精性病因引起的急性肝病患者在细胞溶解酶恢复正常之前不应接受他汀类药物治疗;v)慢性肝炎患者如果心血管风险升高,且能进行仔细随访以快速识别进一步肝损伤的发生,则可使用他汀类药物治疗;vi)受免疫抑制治疗引起的血脂异常影响的肝移植受者可在仔细临床监测下使用他汀类药物治疗;vii)在大多数受非酒精性肝脂肪变性影响的血脂异常患者中,他汀类药物的益处可能超过风险,非酒精性肝脂肪变性是一种在胰岛素抵抗患者中经常诊断出的疾病。

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