Beaumont Health System, Royal Oak, MI, USA.
Ann Pharmacother. 2013 Sep;47(9):1229-33. doi: 10.1177/1060028013500646.
To describe a case of BK virus encephalitis with attempted direct antiviral therapy, review the reported cases of BK virus in the central nervous system, and report the novel use of intravenous cimetidine in place of oral probenecid to minimize the toxicities of intravenous cidofovir.
A 36-year-old male with acute myelomonocytic leukemia and subsequent myelodysplastic syndrome underwent allogeneic hematopoietic stem cell transplant. His course was complicated by severe graft-versus-host disease involving his skin and gastrointestinal tract. Five weeks after transplantation, he developed fever and confusion. Magnetic resonance imaging was suggestive of limbic encephalitis and cerebrospinal fluid tested positive for BK virus. Therapy with intravenous cidofovir was thought to be indicated. Although probenecid is commonly used to minimize the toxicities of cidofovir, the patient's severe graft-versus-host disease raised concerns about absorption of oral medications. Based on animal models and pharmacokinetic data, intravenous cimetidine was used in place of oral probenecid. Despite these therapies, the patient's mental status did not improve. He developed progressive organ system failure, and care was ultimately withdrawn.
BK virus is increasingly described as a cause of encephalitis. The majority of reported cases have occurred in immunocompromised patients and have generally had a poor outcome. This case describes attempted antiviral therapy using cidofovir, the antiviral agent used most frequently in other syndromes due to BK virus. Intravenous cimetidine is a novel modality used to minimize ocular and renal toxicities frequently seen with cidofovir, and we believe this warrants further investigation.
BK virus may be a cause of encephalitis in immunocompromised hosts, and cidofovir represents a possible treatment option. Intravenous cimetidine can be considered to minimize toxicities associated with cidofovir use in patients unable to tolerate or absorb oral probenecid.
描述一例采用直接抗病毒治疗的 BK 病毒脑炎病例,回顾中枢神经系统 BK 病毒的报道病例,并报告静脉西咪替丁替代口服丙磺舒以最小化更昔洛韦静脉毒性的新用途。
一名 36 岁男性,患有急性髓单核细胞白血病和随后的骨髓增生异常综合征,接受了异基因造血干细胞移植。他的病程并发严重的移植物抗宿主病,累及皮肤和胃肠道。移植后 5 周,他出现发热和意识模糊。磁共振成像提示边缘性脑炎,脑脊液 BK 病毒检测阳性。考虑使用更昔洛韦静脉治疗。尽管丙磺舒常用于最小化更昔洛韦的毒性,但患者严重的移植物抗宿主病引起了对口服药物吸收的担忧。基于动物模型和药代动力学数据,使用静脉西咪替丁替代口服丙磺舒。尽管进行了这些治疗,但患者的精神状态仍未改善。他出现进行性多器官系统衰竭,最终停止治疗。
BK 病毒越来越多地被描述为脑炎的病因。大多数报道的病例发生在免疫功能低下的患者中,且通常预后较差。该病例描述了使用更昔洛韦进行抗病毒治疗的尝试,更昔洛韦是其他由于 BK 病毒引起的综合征中最常使用的抗病毒药物。静脉西咪替丁是一种新的方法,用于最小化更昔洛韦常见的眼部和肾脏毒性,我们认为这值得进一步研究。
BK 病毒可能是免疫功能低下宿主脑炎的病因,更昔洛韦是一种可能的治疗选择。对于无法耐受或吸收口服丙磺舒的患者,静脉西咪替丁可用于最小化与更昔洛韦使用相关的毒性。