Bunnell Kristen L, Vibhakar Sonia, Glowacki Robert C, Gallagher Maureen A, Osei Albert M, Huhn Gregory
College of Pharmacy, University of Illinois at Chicago, Chicago, Illinois.
Ruth M. Rothstein CORE Center, Cook Country Health and Hospitals System, Chicago, Illinois.
Pharmacotherapy. 2016 Sep;36(9):e148-53. doi: 10.1002/phar.1803.
Direct-acting antivirals (DAAs) have revolutionized the treatment of hepatitis C virus (HCV) infection, with superior efficacy and safety compared to interferon-based therapies. Despite these improvements, drug interactions with DAAs exist and may be clinically relevant in human immunodeficiency virus (HIV)-coinfected patients. We present a case of nephrotoxicity associated with concomitant use of tenofovir disoproxil fumarate (TDF) and ledipasvir-sofosbuvir (LDV-SOF). A 56-year-old woman with HIV infection who had been taking efavirenz/tenofovir/emtricitabine (EFV/TDF/FTC) for 6 years developed acute kidney injury 8 weeks after initiating LDV-SOF for the treatment of HCV infection. Her serum creatinine concentration peaked at 10 mg/dL, compared with her baseline concentration of 0.9-1 mg/dL. Kidney biopsy revealed acute tubular necrosis and acute interstitial nephritis. Both LDV-SOF and TDF were discontinued, and the patient's serum creatinine concentration decreased to 1.3 mg/dL over the following 6 weeks. We postulate that this adverse drug reaction may have been secondary to the known interaction between ledipasvir and TDF, which results in increased TDF exposure. Despite knowledge of this interaction, LDV-SOF is commonly prescribed in patients with HIV-HCV coinfection, as patients who received LDV-SOF- and TDF-containing regimens in trials have not demonstrated adverse clinical consequences related to this interaction. This case highlights the rare but potentially serious nephrotoxicity that can result from TDF toxicity and serves as a reminder to clinicians to implement close renal function monitoring in patients receiving both LDV-SOF and TDF. Clinicians prescribing LDV-SOF to HCV-HIV-coinfected patients receiving TDF should be cautious about use with concomitant nephrotoxic medications and monitor markers of tubular dysfunction, including urinary phosphorus excretion, and renal injury at baseline and week 4 of therapy. Tenofovir alafenamide and alternative DAAs may also have a role in the management of patients at high risk for renal adverse effects from TDF.
直接作用抗病毒药物(DAAs)彻底改变了丙型肝炎病毒(HCV)感染的治疗方式,与基于干扰素的疗法相比,其疗效和安全性更优。尽管有这些改进,但与DAAs的药物相互作用依然存在,在合并感染人类免疫缺陷病毒(HIV)的患者中可能具有临床相关性。我们报告一例与同时使用替诺福韦酯(TDF)和来迪派韦-索磷布韦(LDV-SOF)相关的肾毒性病例。一名56岁感染HIV的女性,服用依非韦伦/替诺福韦/恩曲他滨(EFV/TDF/FTC)6年,在开始使用LDV-SOF治疗HCV感染8周后发生急性肾损伤。她的血清肌酐浓度峰值达到10mg/dL,而基线浓度为0.9 - 1mg/dL。肾活检显示急性肾小管坏死和急性间质性肾炎。停用LDV-SOF和TDF后,患者的血清肌酐浓度在接下来的6周内降至1.3mg/dL。我们推测这种药物不良反应可能继发于已知的来迪派韦与TDF之间的相互作用,这会导致TDF暴露增加。尽管了解这种相互作用,但LDV-SOF仍常用于HIV-HCV合并感染患者,因为在试验中接受含LDV-SOF和TDF方案的患者未显示出与此相互作用相关的不良临床后果。该病例突出了TDF毒性可能导致的罕见但潜在严重的肾毒性,并提醒临床医生对接受LDV-SOF和TDF的患者进行密切肾功能监测。给接受TDF的HCV-HIV合并感染患者开具LDV-SOF的临床医生,在与具有肾毒性的药物合用时应谨慎,并在基线和治疗第4周监测肾小管功能障碍标志物,包括尿磷排泄和肾损伤情况。替诺福韦艾拉酚胺和其他替代DAAs在管理有TDF导致肾不良反应高风险的患者中可能也有作用。
