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异烟肼-利福平治疗结核病所致肝炎的诱发因素。

Predisposing factors in hepatitis induced by isoniazid-rifampin treatment of tuberculosis.

作者信息

Grönhagen-Riska C, Hellstrom P E, Fröseth B

出版信息

Am Rev Respir Dis. 1978 Sep;118(3):461-6. doi: 10.1164/arrd.1978.118.3.461.

Abstract

Seventy-five patients who developed mild hepatic reactions (serum transaminase concentrations of 45 to 149 units per liter) and 50 patients who showed more serious liver damage (serum transaminase values greater than 150 units per liter) were compared with 261 consecutive patients who had no liver reactions during treatment with rifampin and isoniazid. Generally, liver toxicity occurred in 18 per cent of patients receiving combined anti-tuberculous drug therapy. Small increases in transaminase occurred in 14 per cent of the patients; large increases occurred in 4 per cent. Elderly women comprised a risk group. Among patients exhibiting a more serious hepatic lesion (transaminase values greater than 150 units per liter), alcoholics, mostly men, formed another risk group, together with other patients with a history of previous liver or biliary disease. Of 261 patients who did not develop a liver reaction, 57 per cent were slow INH acetylators. In this study, the groups with small and large increases in transaminase were clearly separated; in the former group there was no preponderance of phenotype, whereas in the latter group, slow acetylators clearly dominated among early (first 4 weeks of treatment) hepatic reactions (P less than 0.01). Studies of single-drug regimens of isoniazid have shown that neither slow nor rapid acetylation has any causal influence on isoniazid-induced hepatitis. Because the metabolism of rifampin is independent of the acetylation process, rifampin and isoniazid in combination seem to cause a toxic hepatitis that differs from the hepatitis induced by either drug separately.

摘要

将75例出现轻度肝脏反应(血清转氨酶浓度为每升45至149单位)的患者和50例显示更严重肝损伤(血清转氨酶值大于每升150单位)的患者,与261例在接受利福平和异烟肼治疗期间未出现肝脏反应的连续患者进行比较。一般来说,接受联合抗结核药物治疗的患者中18%出现肝毒性。14%的患者转氨酶有小幅升高;4%的患者转氨酶大幅升高。老年女性构成一个风险组。在表现出更严重肝脏病变(转氨酶值大于每升150单位)的患者中,酗酒者(大多为男性)与其他有既往肝脏或胆道疾病史的患者一起构成另一个风险组。在261例未出现肝脏反应的患者中,57%是异烟肼慢乙酰化者。在本研究中,转氨酶小幅升高组和大幅升高组明显分开;在前一组中,表型没有优势,而在后一组中,慢乙酰化者在早期(治疗的前4周)肝脏反应中明显占主导(P小于0.01)。对异烟肼单一药物治疗方案的研究表明,慢乙酰化或快乙酰化对异烟肼所致肝炎均无因果影响。由于利福平的代谢独立于乙酰化过程,利福平和异烟肼联合使用似乎会导致一种不同于单独使用任何一种药物所致肝炎的中毒性肝炎。

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