病例报告:体外光疗治疗BK病毒肾病作为一种新的治疗高风险排斥肾移植受者。

Frontiers in nephrology Pub Date : 2025-07-21 eCollection Date: 2025-01-01 DOI:10.3389/fneph.2025.1625060
Marilena Gregorini, Claudia Del Fante, Tefik Islami, Maria Antonietta Grignano, Nicoletta Serpieri, Cesare Perotti, Gianluca Viarengo, Alessia Locurcio, Giuseppe Lanotte, Alessandro Tragni, Emma Diletta Stea, Chiara Martinelli, Alessandro Marchi, Valentina Portalupi, Andreana De Mauri, Elisabetta Margiotta, Eleonora Francesca Pattonieri, Grazia Soccio, Teresa Rampino
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引用次数: 0

摘要

背景:BK病毒相关性肾病(BKVAN)是免疫抑制下潜伏BK病毒(BKV)再激活引起的肾移植的主要并发症。BKVAN与移植物损失增加密切相关。目前,没有有效的抗病毒治疗BKVAN。此外,供体特异性抗体(dsa)的发展和急性和慢性排斥反应的风险使免疫抑制治疗(IS)的减少复杂化。本病例报告阐述了在高度敏感的移植受体中BKVAN的管理,并探讨了体外光造血(ECP)作为免疫调节工具的潜在用途。病例:44岁白人妇女,既往移植失败,多次输血,接受第二次肾移植。由于抗体水平高,患者接受血浆置换、胸腺球蛋白和类固醇诱导治疗,随后使用他克莫司、霉酚酸酯(MMF)和类固醇维持治疗。最初移植物功能良好,活检显示无排斥反应。在第四年,患者出现BKV病毒血症增加(峰值为40,050拷贝/mL), MMF减少,在6个月内清除了BKV。两年后,dsa再次出现,导致MMF增加。2020年8月,患者GFR下降,BKV病毒血症升高(峰值162,000拷贝/mL),移植物活检显示BKVAN。IS减少(停用MMF,他克莫司逐渐减少)。8个月后,病毒血症消失,但抗dr53 dsa (MFI 16000)水平显著升高。由于患者高度敏感且有动静脉瘘血栓形成,不推荐使用mTOR抑制剂。为了在不进一步抑制抗病毒免疫的情况下调节同种异体免疫,引入了ECP。在接下来的两年中,患者表现出稳定的肾功能(eGFR 30-40 mL/min),没有BKV病毒血症复发,dsa滴度逐渐降低。未发生急性排斥反应。结论:在一个高度敏感的BKVAN患者和标准治疗禁忌症中,ECP联合量身定制的免疫抑制方案被证明在控制病毒复制、保持移植物功能和减轻同种免疫风险方面是有效的。考虑到ECP作为复杂BKVAN方案的辅助治疗的潜力,进一步的研究是有必要的。
本文章由计算机程序翻译,如有差异,请以英文原文为准。

Case Report: Extracorporeal photopheresis for BK virus nephropathy as a novel treatment for high-risk rejection kidney transplant recipient.

Case Report: Extracorporeal photopheresis for BK virus nephropathy as a novel treatment for high-risk rejection kidney transplant recipient.

Background: BK virus-associated nephropathy (BKVAN) is a major complication in kidney transplantation caused by the reactivation of latent BK virus (BKV) under immunosuppression. BKVAN has been strongly associated with increased graft loss. Currently, there is no effective antiviral treatment for BKVAN. Additionally, the development of donor-specific antibodies (DSAs) and the risk of acute and chronic rejection complicate the reduction of immunosuppressive therapy (IS). This case report illustrates the management of BKVAN in a highly sensitized transplant recipient and explores the potential use of extracorporeal photopheresis (ECP) as an immunomodulatory tool.

Case: 44-year-old Caucasian woman with a history of failed prior transplant and multiple transfusions underwent a second kidney transplant. Due to a high panel-reactive antibody level, she received induction therapy with plasma exchange, thymoglobulin and steroids, followed by maintenance with tacrolimus, mycophenolate mofetil (MMF), and steroids. Initial graft function was good, and protocol biopsies showed no rejection. In year four, the patient developed an increasing BKV viremia (peak of 40,050 copies/mL) and MMF was reduced, which cleared BKV in six months. Two years later, DSAs reappeared, which led to an increase in MMF. In August 2020 the patient showed a decline of GFR, elevated BKV viremia (peak 162,000 copies/mL), and a graft biopsy was performed revealing BKVAN. IS was reduced (MMF was discontinued, and tacrolimus was tapered). After eight months, the viremia cleared up, but anti-DR53 DSAs (MFI 16000) levels increased significantly. As the patient was highly sensitized and had a thrombosis of arteriovenous fistula, mTOR inhibitors were not recommended. In order to modulate alloimmunity without further suppressing antiviral immunity, ECP was introduced. Over the next two years, the patient showed stable renal function (eGFR 30-40 mL/min), no recurrence of BKV viremia, and a gradual reduction in DSAs titers. No acute rejection episodes occurred.

Conclusions: In a highly sensitized patient with BKVAN and contraindications to standard therapies, ECP combined with a tailored immunosuppressive regimen proved effective in controlling viral replication, preserving graft function, and mitigating alloimmune risks. Considering the potential of ECP as an adjunctive therapy in complex BKVAN scenarios, further investigation is warranted.

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