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抗结核药物与肝毒性。

Antituberculosis drugs and hepatotoxicity.

作者信息

Yew Wing Wai, Leung Chi Chiu

机构信息

Tuberculosis and Chest Unit, Grantham Hospital, Hong Kong, China.

出版信息

Respirology. 2006 Nov;11(6):699-707. doi: 10.1111/j.1440-1843.2006.00941.x.

DOI:10.1111/j.1440-1843.2006.00941.x
PMID:17052297
Abstract

Isoniazid, pyrazinamide and rifampicin have hepatotoxic potential, and can lead to such reactions during antituberculosis chemotherapy. Most of the hepatotoxic reactions are dose-related; some are, however, caused by drug hypersensitivity. The immunogenetics of antituberculosis drug-induced hepatotoxicity, especially inclusive of acetylaor phenotype polymorphism, have been increasingly unravelled. Other principal clinical risk factors for hepatotoxicity are old age, malnutrition, alcoholism, HIV infection, as well as chronic hepatitis B and C infections. Drug-induced hepatic dysfunction usually occurs within the initial few weeks of the intensive phase of antituberculosis chemotherapy. Vigilant clinical (including patient education on symptoms of hepatitis) and biochemical monitoring are mandatory to improve the outcomes of patients with drug-induced hepatotoxicity during antituberculosis chemotherapy. Some fluoroquinolones like ofloxacin/levofloxacin may have a role in constituting non-hepatotoxic drug regimens for management of tuberculosis (TB) in the presence of hepatic dysfunction. Isoniazid administration is currently the standard therapy for latent TB infection. Rifamycins like rifampicin or rifapentine, alone or in combination with isoniazid, may also be considered as alternatives, pending accumulation of further clinical data. During treatment of latent TB infection, regular follow up is essential to ensure adherence to therapy and facilitate clinical monitoring for hepatic dysfunction. Monitoring of liver chemistry is also required for those patients at risk of drug-induced hepatotoxicity.

摘要

异烟肼、吡嗪酰胺和利福平具有肝毒性,在抗结核化疗期间可导致此类反应。大多数肝毒性反应与剂量相关;然而,有些是由药物超敏反应引起的。抗结核药物所致肝毒性的免疫遗传学,尤其是乙酰化酶表型多态性,已越来越多地被揭示。肝毒性的其他主要临床危险因素包括老年、营养不良、酗酒、艾滋病毒感染以及慢性乙型和丙型肝炎感染。药物性肝功能障碍通常发生在抗结核化疗强化期的最初几周内。必须进行警惕的临床监测(包括对患者进行肝炎症状教育)和生化监测,以改善抗结核化疗期间药物性肝毒性患者的治疗结局。在肝功能不全的情况下,一些氟喹诺酮类药物,如氧氟沙星/左氧氟沙星,可能在构成非肝毒性抗结核治疗方案中发挥作用。目前,异烟肼给药是潜伏性结核感染的标准治疗方法。在积累更多临床数据之前,利福霉素类药物,如利福平或利福喷汀,单独使用或与异烟肼联合使用,也可被视为替代方案。在潜伏性结核感染的治疗期间,定期随访对于确保坚持治疗和便于对肝功能障碍进行临床监测至关重要。对于有药物性肝毒性风险的患者,也需要监测肝功能。

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Antituberculosis drugs and hepatotoxicity.抗结核药物与肝毒性。
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