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首页> 外文期刊>Oncoimmunology. >A novel in situ multiplex immunofluorescence panel for the assessment of tumor immunopathology and response to virotherapy in pediatric glioblastoma reveals a role for checkpoint protein inhibition
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A novel in situ multiplex immunofluorescence panel for the assessment of tumor immunopathology and response to virotherapy in pediatric glioblastoma reveals a role for checkpoint protein inhibition

机译:用于评估肿瘤免疫病理学和对儿科胶质母细胞瘤的病毒治疗的评估的新型新型多重免疫荧光板揭示了检查点蛋白抑制的作用

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摘要

Immunotherapy with oncolytic herpes simplex virus-1 therapy offers an innovative, targeted, less-toxic approach for treating brain tumors. However, a major obstacle in maximizing oncolytic virotherapy is a lack of comprehensive understanding of the underlying mechanisms that unfold in CNS tumors/associated microenvironments after infusion of virus. We demonstrate that our multiplex biomarker screening platform comprehensively informs changes in both topographical location and functional states of resident/infiltrating immune cells that play a role in neuropathology after treatment with HSV G207 in a pediatric Phase 1 patient. Using this approach, we identified robust infiltration of CD8+ T cells suggesting activation of the immune response following virotherapy; however there was a corresponding upregulation of checkpoint proteins PD-1, PD-L1, CTLA-4, and IDO revealing a potential role for checkpoint inhibitors. Such work may ultimately lead to an understanding of the governing pathobiology of tumors, thereby fostering development of novel therapeutics tailored to produce optimal responses.
机译:用洋肠疱疹疱疹病毒-1疗法免疫疗法为治疗脑肿瘤提供创新,有针对性的,毒性的方法。然而,最大化溶解的病毒治疗的主要障碍是对缺乏在输注后的CNS肿瘤/相关的微环境中展开的潜在机制缺乏全面了解。我们证明我们的多路复用生物标志物筛查平台全面地通知居民/渗透免疫细胞的地形位置和功能状态的变化,所述居民/渗透免疫细胞在儿科1患者中用HSV G207处理后发挥神经病理学的作用。使用这种方法,我们鉴定了CD8 + T细胞的强大渗透,表明在病毒疗法后激活免疫应答;然而,检查点蛋白Pd-1,PD-L1,CTLA-4和IDO存在相应的上调,揭示检查点抑制剂的潜在作用。这些工作最终可能导致对肿瘤的治疗病病病病病病病病病病病病病病病病病病病病病病病病病病病病病病病病病病病病?,从而培养着针对产生最佳反应的新型治疗剂的发展。

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