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针对持续性病毒感染的细胞免疫疗法揭示了一种独特的从中枢神经系统清除的模式。

Cytoimmunotherapy for persistent virus infection reveals a unique clearance pattern from the central nervous system.

作者信息

Oldstone M B, Blount P, Southern P J, Lampert P W

出版信息

Nature. 1986;321(6067):239-43. doi: 10.1038/321239a0.

Abstract

The mechanism(s) by which infectious or malignant material is cleared by the host has long been an area of intensive study. We have used the murine model of infection with lymphocytic choriomeningitis virus (LCMV) to look at immune clearance during persistent infection. LCMV was selected because the mouse is its natural host, it easily induces acute or persistent infection in vivo, and the mechanism by which it is cleared in vivo during acute infection is now well understood. Clearance, although associated with several antiviral immune effector mechanisms, is primarily dependent on the activity of virus-specific cytotoxic T lymphocytes (CTL) restricted by H-2 molecules of the mouse major histocompatibility complex (MHC). If these cells fail to generate or are depleted, progression from acute to persistent infection occurs. Here, using molecular probes, we show that viral nucleic acid sequences, viral proteins and infectious materials can be efficiently and effectively cleared by adoptive transfer of antiviral H-2-restricted lymphocytes bearing the Lyt 2+ phenotype. Viral materials are cleared from a wide variety of tissues and organs where they normally lodge during persistent infection. Unexpectedly, the mode by which viral materials are removed from the central nervous system (CNS) differed markedly from the mechanism of clearance occurring at other sites. These observations indicate the possible use of adoptive lymphocyte therapy for treatment of persistent infections and suggest that immune clearance of products from the CNS probably occurs by a process distinct from those in other organs.

摘要

宿主清除感染性或恶性物质的机制长期以来一直是深入研究的领域。我们利用淋巴细胞性脉络丛脑膜炎病毒(LCMV)感染的小鼠模型来研究持续性感染期间的免疫清除。选择LCMV是因为小鼠是其天然宿主,它在体内容易诱导急性或持续性感染,并且现在已经清楚地了解了其在急性感染期间在体内被清除的机制。清除虽然与几种抗病毒免疫效应机制有关,但主要依赖于受小鼠主要组织相容性复合体(MHC)的H-2分子限制的病毒特异性细胞毒性T淋巴细胞(CTL)的活性。如果这些细胞未能产生或被耗尽,就会发生从急性感染到持续性感染的进展。在这里,我们使用分子探针表明,通过过继转移具有Lyt 2 +表型的抗病毒H-2限制淋巴细胞,可以有效且高效地清除病毒核酸序列、病毒蛋白和感染性物质。病毒物质从持续性感染期间它们通常驻留的多种组织和器官中被清除。出乎意料的是,病毒物质从中枢神经系统(CNS)中清除的方式与在其他部位发生的清除机制明显不同。这些观察结果表明过继淋巴细胞疗法可能用于治疗持续性感染,并表明中枢神经系统产物的免疫清除可能通过与其他器官不同的过程发生。

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