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神经科患者脑脊液中 BK 病毒相关性感染及不同患者群体中完整 VP1 基因的突变分析。

BK virus-associated infection in cerebrospinal fluid of neurological patients and mutation analysis of the complete VP1 gene in different patient groups.

机构信息

Host-Microbe Interaction Research Group, Department of Medical Biology, Faculty of Health Sciences, University of Tromsø, Tromsø, Norway.

出版信息

J Cell Physiol. 2012 Jan;227(1):136-45. doi: 10.1002/jcp.22711.

DOI:10.1002/jcp.22711
PMID:21374594
Abstract

While BK virus (BKV) is frequently associated with pathological conditions in bone marrow and renal transplant recipients, BKV infection in neurological individuals has been rarely reported. As a result of a BKV, JCV, and SV40 large T antigen-specific multiplex PCR on 2,062 cerebrospinal fluid (CSF) samples from neurological patients suspicious of JCV infection, we identified 20 subjects with at least 1 CSF specimen positive for BKV large T antigen DNA. Because VP1 protein has been suggested to influence the biological/pathological properties of BKV, we tried to sequence the entire VP1 gene in the BKV-positive neurological patients and succeeded in 14 of the 20 neurological patients. To compare the VP1 sequence of the BKV neurological strains with that of non-neurotropic strains in other clinical situations, full-length VP1 DNA was sequenced in 15 renal and 6 bone marrow transplant recipients positive to BKV-viremia, and in 8 pregnant women as non-pathological controls. An increased (respectively, decreased) tendency for mutations in the BC loop (respectively, EF loop) was observed, and no mutations were detected in the CD, GH, and HI loops. Subtype I was predominant (93%) and compared to archetypal BKV (WW), amino acid substitutions were detected in 4/14 neurological patients, 10/15 renal transplant recipients, 3/6 bone marrow transplant patients, and in all the pregnant women. Each patient group had distinctive VP1 mutations, but these unique substitutions were not present in all patients of this group. However, molecular modeling simulations of the VP1 mutants predicted changes in protein surface properties which might affect the VP1-receptor interaction.

摘要

虽然 BK 病毒(BKV)常与骨髓和肾移植受者的病理状况有关,但在神经科患者中 BKV 感染的报道很少。通过对 2062 例疑似 JCV 感染的神经科患者的脑脊液(CSF)样本进行 BKV、JCV 和 SV40 大 T 抗原的多重 PCR,我们发现 20 例 CSF 标本至少有 1 份 BKV 大 T 抗原 DNA 阳性。由于 VP1 蛋白被认为会影响 BKV 的生物学/病理学特性,我们试图对 BKV 阳性的神经科患者的整个 VP1 基因进行测序,在 20 例神经科患者中有 14 例成功测序。为了比较 BKV 神经株与其他临床情况下非神经亲和株的 VP1 序列,我们对 15 例 BKV 血症阳性的肾移植受者和 6 例骨髓移植受者以及 8 例孕妇(非病理对照)的全长 VP1 DNA 进行了测序。在 BC 环(分别为 EF 环)中观察到突变增加(分别减少)的趋势,而在 CD、GH 和 HI 环中未检测到突变。优势型为 I 型(93%),与原型 BKV(WW)相比,在 14 例神经科患者中有 4 例、15 例肾移植受者中有 10 例、6 例骨髓移植受者中有 3 例和所有孕妇中都检测到氨基酸取代。每个患者组都有独特的 VP1 突变,但并非该组所有患者都存在这些独特的取代。然而,VP1 突变体的分子建模模拟预测了蛋白质表面特性的变化,这可能会影响 VP1-受体相互作用。

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