Hepatotoxicity during legacy cancer chemotherapy in patients infected with hepatitis C virus: A retrospective cohort study.

Canadian liver journal Pub Date : 2022-02-04 eCollection Date: 2022-01-01 DOI:10.3138/canlivj-2021-0018
Jean-Luc Szpakowski, Lue-Yen Tucker, David M Baer, Mary Pat Pauly
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引用次数: 1

Abstract

Background: The rates and causes of significant hepatotoxicity with cancer chemotherapy (CCT) in patients infected with hepatitis C virus (HCV) are incompletely characterized.

Methods: We compared rates of grade 3 or 4 hepatotoxicity, defined as elevated transaminases, during CCT in patients who are mono-infected with HCV compared with rates in controls matched on demographics, diagnosis, and rituximab use. We excluded patients with hepatobiliary cancers, hepatitis B virus or human immunodeficiency virus infection. Hepatotoxicity was attributed to a medical cause, cancer progression, or CCT, including HCV flare.

Results: Patients with HCV (n = 196) had a higher rate of cirrhosis than the 1,130 matched controls (21.9% versus 4%; P <0.001). Their higher rate of overall hepatotoxicity (8.7% versus 4.5% of controls, P = 0.01) was due to higher rate of CCT-related hepatotoxicity (4.1% versus 1.2%, P = 0.01). On multivariable analysis, the largest risk factor for overall hepatotoxicity was cirrhosis, and the only risk factor for CCT-related hepatotoxicity was HCV infection. Among those with HCV, the only significant risk factor for hepatotoxicity was rituximab use. Hepatotoxicity caused by CCT delayed or altered treatment in only 3 HCV patients and 1 control (1.5% versus 0.1%, P = 0.01).

Conclusions: Most patients with HCV can safely be treated with cancer chemotherapy. Cirrhosis and HCV infection contributed to increased hepatotoxicity in subjects on CCT. Among HCV patients, rituximab use was the major risk factor for increased hepatotoxicity. Hepatotoxicity due to CCT itself rarely altered or delayed CCT. Nonetheless, HCV-positive patients should be monitored carefully during CCT.

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丙型肝炎病毒感染者传统癌症化疗期间的肝毒性:一项回顾性队列研究。
背景:癌症化疗(CCT)对丙型肝炎病毒(HCV)感染者显著肝毒性的发生率和原因尚不完全清楚。方法:我们比较了单一感染HCV的患者在CCT期间3级或4级肝毒性(定义为转氨酶升高)的发生率与人口统计学、诊断和利妥昔单抗使用匹配的对照组的发生率。我们排除了患有肝胆癌、乙型肝炎病毒或人类免疫缺陷病毒感染的患者。肝毒性归因于医学原因、癌症进展或CCT,包括HCV发作。结果:HCV患者(n=196)的肝硬化发生率高于1130名匹配的对照组(21.9%对4%;P=0.01),这是由于CCT相关肝毒性发生率较高(4.1%对1.2%,P=0.01)。多变量分析显示,总体肝毒性的最大危险因素是肝硬化,而CCT相关的肝毒性的唯一危险因素是HCV感染。在HCV患者中,肝毒性的唯一重要危险因素是利妥昔单抗的使用。CCT引起的肝毒性仅在3例HCV患者和1例对照组中延迟或改变治疗(1.5%对0.1%,P=0.01)。结论:大多数HCV患者可以安全地接受癌症化疗。肝硬化和丙型肝炎病毒感染导致CCT受试者肝毒性增加。在HCV患者中,使用利妥昔单抗是肝毒性增加的主要危险因素。CCT本身引起的肝毒性很少改变或延迟CCT。尽管如此,HCV阳性患者应在CCT期间仔细监测。
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