抗结核药物所致肝毒性的发生率及危险因素评估

Incidence of hepatotoxicity due to antitubercular medicines and assessment of risk factors.

作者信息

Shakya Rajani, Rao B Subba, Shrestha Bhawana

机构信息

Department of Pharmacy, Kathmandu University, Dhulikhel, Nepal.

出版信息

Ann Pharmacother. 2004 Jun;38(6):1074-9. doi: 10.1345/aph.1D525. Epub 2004 Apr 30.

DOI:10.1345/aph.1D525

PMID:15122004

Abstract

BACKGROUND

Antitubercular drugs cause derangement of hepatic function revealed by clinical examination and abnormal liver function test results. Potential hepatotoxicity of some of the first-line antitubercular agents remains a problem, especially during the initial period of treatment.

OBJECTIVE

To determine the incidence of antitubercular drug-induced hepatotoxicity in a Nepalese urban population and assess the risk factors.

METHOD

Fifty patients diagnosed with active tuberculosis infection with normal pretreatment liver function were monitored clinically as well as biochemically in a prospective cohort analysis.

RESULTS

Antitubercular drugs were found to be associated with derangement of hepatic function, resulting in elevation of liver enzymes to a variable extent (t = -4.550, p < 0.01 for aspartate aminotransferase [AST]; t = -5.467, p < 0.01 for alanine aminotransferase [ALT] at 95% CI). Thirty-eight percent of patients had 2 times and 30% had >3 times elevation of ALT. Similarly, 40% and 29% of patients showed 2 and >3 times elevation of the AST level, respectively. Four patients (8%) developed drug-induced hepatotoxicity. Jaundice was the presenting symptom in all patients. The time interval for onset of hepatotoxicity after initiation of therapy was 12-60 days (median 28). Antitubercular drug-induced hepatotoxicity was found more often in younger patients (6% vs 2%; p = 0.368, OR 2.75). Female gender was also a higher risk (p = 0.219, OR 4.2). Most patients who had developed hepatitis were diagnosed per sputum-smear positive reactions. Nutritional status, assessed by body mass index and serum albumin level, was the next predisposing factor.

CONCLUSIONS

A finding of an 8% incidence of hepatotoxicity is considerably high. Risk factors of hepatotoxicity included female gender, disease extent, and poor nutritional status. Timely detection and temporary withdrawal of the offending agent can completely cure antitubercular drug-induced hepatotoxicity.

摘要

背景

抗结核药物可导致肝功能紊乱，通过临床检查和肝功能测试结果异常得以揭示。一些一线抗结核药物潜在的肝毒性仍是一个问题，尤其是在治疗初期。

目的

确定尼泊尔城市人群中抗结核药物所致肝毒性的发生率，并评估危险因素。

方法

对50例诊断为活动性结核感染且治疗前肝功能正常的患者进行前瞻性队列分析，进行临床和生化监测。

结果

发现抗结核药物与肝功能紊乱有关，导致肝酶不同程度升高（天冬氨酸氨基转移酶[AST]：t = -4.550，P < 0.01；丙氨酸氨基转移酶[ALT]：t = -5.467，95%可信区间时P < 0.01）。38%的患者ALT升高2倍，30%的患者ALT升高超过3倍。同样，40%和29%的患者AST水平分别升高2倍和超过3倍。4例患者（8%）发生药物性肝毒性。黄疸是所有患者的首发症状。治疗开始后肝毒性出现的时间间隔为12 - 60天（中位数28天）。抗结核药物所致肝毒性在年轻患者中更常见（6%对2%；P = 0.368，比值比2.75）。女性也是较高风险因素（P = 0.219，比值比4.2）。大多数发生肝炎的患者通过痰涂片阳性反应确诊。通过体重指数和血清白蛋白水平评估的营养状况是下一个易感因素。