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不同结构类型无环核苷膦酸酯类化合物对人原代肾细胞中 BK 病毒的作用。

Activities of different classes of acyclic nucleoside phosphonates against BK virus in primary human renal cells.

机构信息

Rega Institute for Medical Research, KU Leuven, Minderbroedersstraat 10, 3000 Leuven, Belgium.

出版信息

Antimicrob Agents Chemother. 2011 May;55(5):1961-7. doi: 10.1128/AAC.01809-10. Epub 2011 Feb 22.

Abstract

BK virus (BKV), a virus belonging to the polyomavirus family, is a circular double-stranded DNA virus that causes nephropathies in immunocompromised patients after kidney or bone marrow transplantation. The occurrence of polyomavirus-associated nephropathy in kidney transplant patients may trigger graft loss, and guidelines for the management of BKV infection have not yet been clearly established. Treatment of BKV nephropathy with cidofovir (CDV) {(S)-1-[3-hydroxy-2-(phosphonomethoxy)propyl]cytosine (HPMPC)}, an acyclic phosphonate analogue of dCMP with a broad antiviral activity against DNA virus infections, has been proposed. The benefit of this small-molecule-based treatment has been evaluated only with a limited number of cases. In this study, we report the evaluation of three different classes of acyclic nucleoside phosphonates for their activities against BKV replication in two different primary renal cells: renal proximal tubular epithelial cells (RPTECs) and human renal cortical epithelial (HRCE) cells. The data indicate that besides HPMPC and its cyclic form, (S)-1-[3-hydroxy-2-(phosphonomethoxy)propyl]-5-azacytosine (HPMP-5-azaC), cyclic HPMP (cHPMP)-5-azaC, hexadecyloxyethyl (HDE)-cHPMP-5-azaC, and 9-[2-(phosphonomethoxy)ethyl]guanine (PMEG) are the most selective inhibitors of BKV replication. On the contrary, leflunomide, which has also been proposed for the management of BKV-associated diseases, is not able to inhibit BKV replication at nontoxic concentrations.

摘要

BK 病毒(BKV)属于多瘤病毒科,是一种环状双链 DNA 病毒,在肾或骨髓移植后的免疫功能低下患者中可引起肾病。肾移植患者发生多瘤病毒相关性肾病可能导致移植物丢失,并且尚未明确制定 BKV 感染的管理指南。用西多福韦(CDV)[(S)-1-[3-羟基-2-(膦酸甲酯基)丙基]胞嘧啶(HPMPC)]治疗 BKV 肾病,CDV 是一种具有广泛抗 DNA 病毒感染活性的无环膦酸酯类似物,已被提出。这种基于小分子的治疗的益处仅在有限数量的病例中进行了评估。在这项研究中,我们报告了对三种不同类别的无环核苷膦酸酯在两种不同的原代肾细胞(肾近端小管上皮细胞(RPTEC)和人肾皮质上皮(HRCE)细胞)中对 BKV 复制的活性进行评估。数据表明,除了 HPMPC 和其环形式(S)-1-[3-羟基-2-(膦酸甲酯基)丙基]-5-氮杂胞嘧啶(HPMP-5-azaC)、环 HPMP(cHPMP)-5-azaC、十六烷氧基乙基(HDE)-cHPMP-5-azaC 和 9-[2-(膦酸甲酯基)乙基]鸟嘌呤(PMEG)外,它们还是 BKV 复制的最选择性抑制剂。相反,曾被提议用于治疗 BKV 相关疾病的来氟米特在非毒性浓度下不能抑制 BKV 复制。

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