BK polyomavirus infection: more than 50 years and still a threat to kidney transplant recipients

Sandesh Parajuli, Fahad Aziz, Weixiong Zhong, A. Djamali
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Abstract

BK polyomavirus (BKPyV) is a ubiquitous human polyomavirus and a major infection after kidney transplantation, primarily due to immunosuppression. BKPyV reactivation can manifest as viruria in 30%–40%, viremia in 10%–20%, and BK polyomavirus-associated nephropathy (BKPyVAN) in 1%–10% of recipients. BKPyVAN is an important cause of kidney graft failure. Although the first case of BKPyV was identified in 1971, progress in its management has been limited. Specifically, there is no safe and effective antiviral agent or vaccine to treat or prevent the infection. Even in the current era, the mainstay approach to BKPyV is a reduction in immunosuppression, which is also limited by safety (risk of de novo donor specific antibody and rejection) and efficacy (graft failure). However, recently BKPyV has been getting more attention in the field, and some new treatment strategies including the utilization of viral-specific T-cell therapy are emerging. Given all these challenges, the primary focus of this article is complications associated with BKPyV, as well as strategies to mitigate negative outcomes.
BK 多瘤病毒感染:50 多年来仍对肾移植受者构成威胁
BK 多瘤病毒(BKPyV)是一种无处不在的人类多瘤病毒,也是肾移植后的一种主要感染,这主要是由于免疫抑制造成的。30%-40% 的受者会出现 BKPyV 再激活,10%-20% 的受者会出现病毒血症,1%-10% 的受者会出现 BK 多瘤病毒相关性肾病(BKPyVAN)。BKPyVAN 是导致肾移植失败的一个重要原因。虽然第一例 BKPyV 病例是在 1971 年发现的,但其治疗进展有限。具体来说,目前还没有安全有效的抗病毒药物或疫苗来治疗或预防感染。即使在当今时代,治疗 BKPyV 的主要方法也是减少免疫抑制,但这也受到安全性(产生新的供体特异性抗体和排斥反应的风险)和有效性(移植物失败)的限制。不过,最近 BKPyV 在该领域受到越来越多的关注,一些新的治疗策略正在出现,包括利用病毒特异性 T 细胞疗法。鉴于所有这些挑战,本文的主要重点是与 BKPyV 相关的并发症以及减轻不良后果的策略。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
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