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首例人类抗 JCPyV/VP1 中和单克隆抗体的克隆:表位定义及其在那他珠单抗治疗患者风险分层中的意义。

Cloning of the first human anti-JCPyV/VP1 neutralizing monoclonal antibody: epitope definition and implications in risk stratification of patients under natalizumab therapy.

机构信息

Laboratorio di Microbiologia e Virologia, Università "Vita-Salute" San Raffaele, Milan, Italy.

Laboratorio di Microbiologia e Virologia, Università "Vita-Salute" San Raffaele, Milan, Italy.

出版信息

Antiviral Res. 2014 Aug;108:94-103. doi: 10.1016/j.antiviral.2014.05.017. Epub 2014 Jun 5.

DOI:10.1016/j.antiviral.2014.05.017
PMID:24909571
Abstract

JC virus (JCPyV) has gained novel clinical importance as cause of progressive multifocal leukoencephalopathy (PML), a rare demyelinating disease recently associated to immunomodulatory drugs, such as natalizumab used in multiple sclerosis (MS) cases. Little is known about the mechanisms leading to PML, and this makes the need of PML risk stratification among natalizumab-treated patients very compelling. Clinical and laboratory-based risk-stratification markers have been proposed, one of these is represented by the JCPyV-seropositive status, which includes about 54% of MS patients. We recently proposed to investigate the possible protective role of neutralizing humoral immune response in preventing JCPyV reactivation. In this proof-of-concept study, by cloning the first human monoclonal antibody (GRE1) directed against a neutralizing epitope on JCPyV/VP1, we optimized a robust anti-JCPyV neutralization assay. This allowed us to evaluate the neutralizing activity in JCPyV-positive sera from MS patients, demonstrating the lack of correlation between the level of anti-JCPyV antibody and anti-JCPyV neutralizing activity. Relevant consequences may derive from future clinical studies induced by these findings; indeed the study of the serum anti-JCPyV neutralizing activity could allow not only a better risk stratification of the patients during natalizumab treatment, but also a better understanding of the pathophysiological mechanisms leading to PML, highlighting the contribution of peripheral versus central nervous system JCPyV reactivation. Noteworthy, the availability of GRE1 could allow the design of novel immunoprophylactic strategies during the immunomodulatory treatment.

摘要

JC 病毒(JCPyV)作为进行性多灶性白质脑病(PML)的病因,具有新的临床重要性,PML 是一种罕见的脱髓鞘疾病,最近与免疫调节药物相关,如多发性硬化症(MS)患者中使用的那他珠单抗。导致 PML 的机制知之甚少,这使得对接受那他珠单抗治疗的患者进行 PML 风险分层的需求非常迫切。已经提出了基于临床和实验室的风险分层标志物,其中之一是 JCPyV 血清阳性状态,这包括约 54%的 MS 患者。我们最近提出研究中和性体液免疫反应在预防 JCPyV 再激活中的可能保护作用。在这项概念验证研究中,通过克隆针对 JCPyV/VP1 上中和表位的第一个人类单克隆抗体(GRE1),我们优化了一种强大的抗 JCPyV 中和测定法。这使我们能够评估来自 MS 患者的 JCPyV 阳性血清中的中和活性,证明了抗 JCPyV 抗体水平与抗 JCPyV 中和活性之间缺乏相关性。这些发现可能会导致未来的临床研究产生相关影响;事实上,研究血清抗 JCPyV 中和活性不仅可以在接受那他珠单抗治疗期间更好地对患者进行风险分层,还可以更好地了解导致 PML 的病理生理机制,突出外周与中枢神经系统 JCPyV 再激活的贡献。值得注意的是,GRE1 的可用性可以为免疫调节治疗期间的新型免疫预防策略设计提供帮助。

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