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拉替拉韦、替诺福韦和恩曲他滨治疗 HIV 合并 HCV 慢性肝炎、NNRTI 不耐受和蛋白酶抑制剂诱导的严重肝毒性的患者。

Raltegravir, tenofovir, and emtricitabine in an HIV-infected patient with HCV chronic hepatitis, NNRTI intolerance and protease inhibitors-induced severe liver toxicity.

机构信息

Clinic of Infectious Diseaes, Department of Medicine and Immunology, University of Cagliari, Italy.

出版信息

Eur J Med Res. 2010 Feb 26;15(2):81-3. doi: 10.1186/2047-783x-15-2-81.

Abstract

BACKGROUND

In HIV-infected patients with HCV-related chronic hepatitis, liver impairment and drug toxicity may substantially reduce the number of possible therapeutic options.

CASE DESCRIPTION

we here describe the case of an HCV-HIV coinfected woman who had repeated severe episodes of drug-related liver toxicity with indinavir, saquinavir, fosamprenavir, and darunavir, with minimal further therapeutic options left in this class. Previous treatment-limiting side effects with efavirenz and nevirapine also precluded use of non-nucleoside reverse transcriptase inhibitors. Introduction of an integrase-inhibitor regimen based on raltegravir, tenofovir, and emtricitabine allowed a prompt achievement of undetectable viral load and a substantial rise of CD4 count to high levels, with no subsequent episodes of hepatic toxicity, and no other side effects.

CONCLUSIONS

given the relatively common prevalence of HCV-related chronic hepatitis among people with HIV, raltegravir might represent an important alternative option for a substantial number of patients who cannot be treated with protease inhibitors or NNRTI because of drug-related hepatic toxicity.

摘要

背景

在 HIV 感染合并 HCV 相关慢性肝炎的患者中,肝损伤和药物毒性可能会大大减少可能的治疗选择。

病例描述

我们在此描述了一位 HCV/HIV 合并感染的女性患者,她曾因使用茚地那韦、沙奎那韦、福沙那韦和达芦那韦而出现反复严重的药物相关肝毒性,而此类药物中仅剩有限的治疗选择。先前使用依非韦伦和奈韦拉平的治疗限制副作用也排除了使用非核苷类逆转录酶抑制剂的可能性。基于拉替拉韦、替诺福韦和恩曲他滨的整合酶抑制剂方案的引入,迅速实现了病毒载量不可检测和 CD4 计数大幅升高至高水平,且无后续肝毒性,也无其他副作用。

结论

鉴于 HIV 感染者中 HCV 相关慢性肝炎的相对常见患病率,对于因药物相关肝毒性而无法使用蛋白酶抑制剂或 NNRTI 治疗的大量患者,拉替拉韦可能是一个重要的替代选择。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/845c/3352050/9d1f541aa0d5/2047-783X-15-2-81-1.jpg

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