Clinical features of liver injury induced by anti-tuberculosis drugs and related risk factors
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摘要:
目的 总结分析抗结核药物导致肝损伤的临床特征及危险因素。 方法 选取2017年1月—2018年12月在深圳市第三人民医院诊断为抗结核药物导致肝损伤的129例住院患者,分为肝功能异常组51例(39.53%),药物性肝损伤组78例(60.47%),其中肝衰竭13例(10.08%)。回顾性分析患者的实验室指标、治疗和预后资料。计数资料两组间比较采用χ2检验,正态分布的计量资料两组间比较采用独立样本t检验,非正态分布的计量资料两组间比较采用Mann-Whitney U秩和检验。通过多因素logistic回归分析药物性肝损伤、肝衰竭的风险因素。 结果 药物性肝损伤组和肝功能指标异常组间合并慢性HBV感染比例(χ2=5.616,P=0.018)、无症状肝损伤比例(χ2=9.451,P=0.002)、肝衰竭比例(χ2=9.453,P=0.002)、需调整抗结核方案比例(χ2=16.787,P<0.001)、首次肝损伤时间(Z=-4.001, P<0.001)、肝功能恢复时间(Z=-1.735, P<0.001)、肝性脑病比例(χ2=4.114,P=0.043)比较,差异均有统计学意义。多因素logistic回归分析显示,首次肝损伤时间>8周(OR=3.94, 95%CI: 1.02~15.25, P=0.047)、无症状肝损伤(OR=7.64, 95%CI: 1.63~35.86,P=0.010)是发生药物性肝损伤的独立危险因素。合并慢性HBV感染(OR=14.42, 95%CI: 2.66~78.09,P=0.002)、首次肝损伤时间>8周(OR=11.97, 95%CI: 2.03~70.50,P=0.006)是发生肝衰竭的独立危险因素,Alb≥35 g/L(OR=0.07, 95%CI: 0.01~0.51,P=0.010)是其保护因素。 结论 抗结核药物会导致严重肝损伤,合并HBV感染、无症状肝损伤、发现肝损伤时间晚、低蛋白会增加严重肝损伤发生风险。定期随访、肝功能监测、适当营养支持和HBV筛查对降低抗结核期间的肝损伤风险具有重要意义。 -
关键词:
- 化学性与药物性肝损伤 /
- 结核 /
- 抗结核药 /
- 疾病特征 /
- 危险因素
Abstract:Objective To investigate the clinical features of liver injury induced by anti-tuberculosis drugs and related risk factors. Methods A total of 129 patients who were diagnosed with liver injury induced by anti-tuberculosis drugs in Shenzhen Third People's Hospital from January 2017 to December 2018 were enrolled and divided into abnormal liver function group with 51 patients (39.53%) and drug-induced liver injury (DILI) group with 78 patients (60.47%), and among these 129 patients, 13 (10.08%) had liver failure. A retrospective analysis was performed for their laboratory markers as well as treatment and prognosis data. The chi-square test was used for comparison of categorical data between two groups; the independent samples t-test was used for comparison of normally distributed continuous data between two groups, and the Mann-Whitney U test was used for comparison of non-normally distributed continuous data between two groups. The multivariable logistic regression model was used to investigate the risk factors for DILI and liver failure. Results There were significant differences between the DILI group and the abnormal liver function group in chronic HBV co-infection (χ2=5.616, P=0.018), asymptomatic liver injury (χ2=9.451, P=0.002), liver failure (χ2=9.453, P=0.002), need to adjust anti-tuberculosis regimen (χ2=16.787, P < 0.001), time to identification of liver injury (Z=-4.001, P < 0.001), time to liver function recovery (Z=-1.735, P < 0.001), and hepatic encephalopathy (χ2=4.114, P=0.043). The multivariate logistic regression analysis showed that time to identification of liver injury > 8 weeks (odds ratio [OR]=3.94, 95% confidence interval [CI]: 1.02-15.25, P=0.047) and asymptomatic liver injury (OR=7.64, 95% CI: 1.63-35.86, P=0.010) were independent risk factors for DILI; chronic HBV co-infection (OR=14.42, 95% CI: 2.66-78.09, P=0.002) and time to identification of liver injury > 8 weeks (OR=11.97, 95% CI: 2.03-70.50, P=0.006) were independent risk factors for liver failure, while albumin ≥35 g/L (OR=0.07, 95% CI: 0.01-0.51, P=0.010) was a protective factor. Conclusion Anti-tuberculosis drugs may induce severe liver injury, and HBV co-infection, asymptomatic liver injury, long time to identification of liver injury, and low albumin level may increase the risk of severe liver injury. Regular follow-up, liver function monitoring, appropriate nutritional support, and HBV screening are important for reducing the risk of liver injury during anti-tuberculosis therapy. -
表 1 患者基本特征
指标 总体(n=129) 肝功能指标异常组(n=51) 药物性肝损伤组(n=78) 统计值 P值 男/女(例) 95/34 41/10 54/24 χ2=1.979 0.159 年龄(岁) 37.0(28.0~51.0) 34.0(26.5~49.0) 40.0(31.0~53.7) Z=-1.528 0.058 合并慢性HBV感染[例(%)] 26(20.2) 5(9.8) 21(26.9) χ2=5.616 0.018 无症状肝损伤[例(%)] 21(16.3) 2(3.9) 19(24.4) χ2=9.451 0.002 首次肝损伤时间(d) 21.0(9.0~45.0) 12.0(7.0~20.5) 30.0(14.0~63.8) Z=-4.001 <0.001 肝功能恢复时间(d) 17.0(11.0~35.0) 12.0(8.0~22.5) 20.0(14.0~45.8) Z=-1.735 <0.001 需调整抗结核药[例(%)] 111(86.1) 36(70.6) 75(96.2) χ2=16.787 <0.001 肝衰竭[例(%)] 13(10.1) 0 13(16.7) χ2=9.453 0.002 肝性脑病[例(%)] 6(4.7) 0 6(7.7) χ2=4.114 0.043 腹水[例(%)] 13(10.1) 1(2.0) 12(15.4) χ2=6.132 0.013 腹膜炎[例(%)] 5(3.9) 0 5(6.4) χ2=3.401 0.065 肝肾综合征[例(%)] 2(1.6) 0 2(2.6) χ2=1.328 0.249 人工肝[例(%)] 10(7.8) 0 10(12.3) χ2=7.088 0.008 死亡[例(%)] 8(6.2) 0 8(10.3) χ2=5.577 0.018 因肝病死亡[例(%)] 6(4.7) 0 6(7.7) χ2=4.114 0.043 表 2 肝损伤程度分组实验室检查结果比较
指标 肝功能指标异常组(n=51) 药物性肝损伤组(n=78) 统计值 P值 首次肝损伤时 INR 1.0(1.0~1.1) 1.1(1.0~1.2) Z=-2.654 0.023 ALT(U/L) 74.4(58.0~106.5) 325.5(138.5~655.0) Z=-7.691 <0.001 AST(U/L) 79.0(58.0~104.0) 275.5(126.3~507.3) Z=-5.064 <0.001 ALP(U/L) 85.0(67.5~108.0) 108.0(85.0~147.0) Z=-2.218 0.021 GGT(U/L) 77.0(41.9~120.0) 96.5(62.3~192.8) Z=-3.351 0.008 TBil(μmol/L) 9.5(6.2~12.8) 19.0(9.5~41.8) Z=-3.702 <0.001 DBil(μmol/L) 3.6(2.3~5.4) 8.4(3.2~18.1) Z=-3.302 <0.001 Alb(g/L) 37.8±6.3 37.0±5.5 t=0.749 0.443 停抗结核药时 INR 1.0(1.0~1.1) 1.1(1.0~1.2) Z=-2.830 0.007 ALT(U/L) 96.0(70.0~125.5) 367.0(208.0~731.3) Z=-7.990 <0.001 AST(U/L) 97.0(77.3~131.5) 295.0(190.0~565.1) Z=-5.140 <0.001 ALP(U/L) 82.0(68.0~108.0) 108.0(85.0~156.5) Z=-2.262 0.017 GGT(U/L) 65.0(41.9~112.0) 105.0(68.3~192.5) Z=-3.214 0.004 TBil(μmol/L) 10.5(7.4~15.3) 19.4(11.1~53.0) Z=-3.651 <0.001 DBil(μmol/L) 3.8(2.6~7.8) 8.8(3.6~26.8) Z=-3.696 <0.001 Alb(g/L) 38.1±6.4 36.8±6.0 t=1.050 0.282 肝损伤高峰时 INR 1.0(1.0~1.1) 1.1(1.0~1.3) Z=-2.824 0.030 ALT(U/L) 97.0(70.0~127.5) 441.30(223.3~777.5) Z=-8.897 <0.001 AST(U/L) 90.0(66.0~124.8) 317.0(197.8~644.1) Z=-5.689 <0.001 ALP(U/L) 85.0(71.0~108.0) 116.5(88.5~194.0) Z=-2.787 0.003 GGT(U/L) 84.0(51.5~130.0) 115.5(70.8~228.8) Z=-3.439 0.004 TBil(μmol/L) 10.4(7.3~15.3) 22.8(11.5~94.3) Z=-4.461 <0.001 DBil(μmol/L) 3.9(2.9~7.9) 9.4(4.0~54.5) Z=-4.617 <0.001 Alb(g/L) 37.3±6.8 35.6±6.6 t=0.725 0.147 肌酐(μmol/L) 62.0(52.0~69.7) 63.5(53.0~72.1) Z=-1.167 0.245 表 3 合并慢性HBV感染者治疗及预后
指标 肝功能指标异常组(n=5) 药物性肝损组(n=21) χ2值 P值 HBeAg[例(%)] 0.014 0.907 阴性 3(60.00) 12(57.14) 阳性 2(40.00) 9(42.86) 抗HBV治疗[例(%)] 2(40.00) 16(76.19) 2.483 0.115 抗结核前启动抗病毒[例(%)] 2(40.00) 1(4.76) 4.913 0.027 肝损后启动抗病毒[例(%)] 0 15(71.43) 8.442 0.004 抗HBV治疗[例(%)] 7.491 0.024 恩替卡韦 0 14 (66.67) 替诺福韦 2 (40.00) 2 (9.52) 人工肝[例(%)] 0 8 (38.10) 2.751 0.097 因肝病死亡[例(%)] 0 4 (19.05) 1.126 0.289 表 4 药物性肝损伤、肝衰竭风险因素分析
参数 例数 单因素分析 多因素分析 OR 95%CI P值 OR 95%CI P值 药物性肝损伤 慢性HBV感染 26 3.39 1.19~9.68 0.023 2.16 0.66~7.04 0.203 女性 34 1.82 0.79~4.23 0.163 2.05 0.81~5.17 0.129 首次肝损伤时间>8周 25 6.29 1.77~22.30 0.004 3.94 1.02~15.25 0.047 Alb≥35 g/L 90 0.80 0.37~1.75 0.578 0.77 0.33~1.80 0.542 ≥60岁 24 1.75 0.67~4.58 0.253 2.00 0.71~5.66 0.190 无症状肝损伤 21 7.89 1.75~35.55 0.007 7.64 1.63~35.86 0.010 肝衰竭 慢性HBV感染 26 20.83 5.17~83.98 <0.001 14.42 2.66~78.09 0.002 女性 34 0.82 0.21~3.19 0.778 1.28 0.20~7.99 0.795 首次肝损伤时间>8周 25 14.06 3.87~51.12 <0.001 11.97 2.03~70.50 0.006 Alb≥35 g/L 90 0.16 0.04~0.54 0.003 0.07 0.01~0.51 0.010 ≥60岁 24 0.78 0.16~3.76 0.754 0.90 0.13~6.43 0.914 无症状肝损伤 21 0.93 0.19~4.53 0.927 1.08 0.11~10.44 0.947 -
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