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抗病毒性肝炎药物与抗逆转录病毒药物的相互作用。

Antiviral hepatitis and antiretroviral drug interactions.

作者信息

Perronne Christian

机构信息

Unité des Maladies Infectieuses et Tropicales, Hôpital Universitaire Raymond Poincaré, Université de Versailles-Saint Quentin, 92380 Garches, France.

出版信息

J Hepatol. 2006;44(1 Suppl):S119-25. doi: 10.1016/j.jhep.2005.11.025. Epub 2005 Dec 1.

Abstract

More and more HIV-infected patients are treated for viral hepatitis, increasing interactions. HEPATITIS C: The concomitant use of didanosine and ribavirin increases the risk of mitochondrial toxicity, responsible for pancreatitis and/or lactic acidosis. Lactic acidosis is characterized by a high mortality rate. Thus, didanosine, but also stavudine, should not be co-administered with ribavirin. Cases of hepatic decompensation have been reported in cirrhotics concomitantly receiving ribavirin and didanosine. Thus, this co-admininistration should be contraindicated in patients with advanced liver fibrosis. Anemia is a frequent side effect of ribavirin. In patients with zidovudine-related anemia, this drug should be discontinued before prescribing ribavirin. Erythropoietin may help to improve the haemoglobin level. HEPATITIS B: Adefovir significantly decreases the plasma levels of saquinavir. Pancreatitis may occur with the co-administration of didanosine and tenofovir. Thus this co-administration should be avoided. Atazanavir concentrations are decreased when tenofovir is co-administered. Thus, atazanavir should be boosted with ritonavir, when combined with tenofovir. Atazanavir increases the concentrations of tenofovir, with the potential risk of increasing the adverse events of tenofovir, including renal disorders. Tenofovir area under the curve is increased if lopinavir-ritonavir are co-administered. The main interactions, with a fatal risk, are observed with didanosine, when co-administered with ribavirin (hepatitis C) or with tenofovir (hepatitis B). Anemia is frequent, but usually moderate, when zidovudine is co-administered with ribavirin. Other interactions are usually easy to manage.

摘要

越来越多的HIV感染患者接受病毒性肝炎治疗,这增加了药物相互作用的情况。丙型肝炎:去羟肌苷与利巴韦林联用会增加线粒体毒性风险,可导致胰腺炎和/或乳酸性酸中毒。乳酸性酸中毒的死亡率很高。因此,去羟肌苷以及司他夫定均不应与利巴韦林联用。已有报告称,同时接受利巴韦林和去羟肌苷治疗的肝硬化患者出现了肝失代偿情况。因此,晚期肝纤维化患者应禁用这种联合用药。贫血是利巴韦林常见的副作用。对于齐多夫定相关贫血患者,在开具利巴韦林处方前应停用该药。促红细胞生成素可能有助于提高血红蛋白水平。乙型肝炎:阿德福韦可显著降低沙奎那韦的血浆水平。去羟肌苷与替诺福韦联用可能会发生胰腺炎。因此应避免这种联合用药。替诺福韦与阿扎那韦联用时阿扎那韦浓度会降低。因此,阿扎那韦与替诺福韦联用时应与利托那韦联用进行增效。阿扎那韦会增加替诺福韦的浓度,可能增加替诺福韦的不良事件风险,包括肾脏疾病。洛匹那韦-利托那韦与替诺福韦联用时,替诺福韦的曲线下面积会增加。与去羟肌苷相关的主要相互作用存在致命风险,即与利巴韦林(丙型肝炎)或替诺福韦(乙型肝炎)联用时。齐多夫定与利巴韦林联用时贫血很常见,但通常为中度。其他相互作用通常易于处理。

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