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Immunotherapeutic strategies to prevent and treat human herpesvirus 6 reactivation after allogeneic stem cell transplantation

机译:异体干细胞移植后预防和治疗人疱疹病毒6活化的免疫治疗策略

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摘要

Human herpesvirus (HHV) 6 causes substantial morbidity and mortality in the immunocompromised host and has no approved therapy. Adoptive transfer of virus specific T cells has proven safe and apparently effective as prophylaxis and treatment of other virus infections in immunocompromised patients; however, extension to subjects with HHV6 has been hindered by the paucity of information on targets of cellular immunity. We now characterize the cellular immune response from 20 donors against 5 major HHV6B antigens predicted to be immunogenic and define a hierarchy of immunodominance of antigens based on the frequency of responding donors and the magnitude of the T-cell response. We identified specific epitopes within these antigens and expanded the HHV6 reactive T cells using a GMP-compliant protocol. The expanded population comprised both CD4+ and CD8+ T cells that were able to produce multiple effector cytokines and kill both peptide-loaded and HHV6B wild-type virus-infected target cells. Thus, we conclude that adoptive T-cell immunotherapy for HHV6 is a practical objective and that the peptide and epitope tools we describe will allow such cells to be prepared, administered, and monitored in human subjects.
机译:人疱疹病毒(HHV)6在免疫功能低下的宿主中引起大量发病和死亡,并且没有经过批准的疗法。事实证明,过继转移病毒特异性T细胞对于预防和治疗免疫受损患者中的其他病毒感染是安全且显然有效的。然而,由于缺乏有关细胞免疫靶标的信息,阻碍了HHV6的推广。现在,我们表征了来自20个供体的5种主要HHV6B抗原的细胞免疫应答,这些抗原预计具有免疫原性,并根据响应性供体的频率和T细胞应答的大小,定义了抗原的免疫优势层次。我们鉴定了这些抗原中的特定表位,并使用符合GMP的协议扩展了HHV6反应性T细胞。扩增后的种群包括CD4 + 和CD8 + T细胞,它们能够产生多种效应细胞因子,并杀死载有肽和被HHV6B野生型病毒感染的靶细胞。因此,我们得出结论,针对HHV6的过继T细胞免疫疗法是一个实际目标,我们描述的肽和表位工具将允许在人类受试者中制备,施用和监测此类细胞。

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