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Natural killer cells and regulatory T cells: how to manipulate a graft for optimal GVL

机译:天然杀伤细胞和调节性T细胞:如何操纵移植物以获得最佳GVL

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摘要

Two of the major complications that limit the efficacy of allogeneic hematopoietic cell transplantation (allo-HCT) are disease relapse and GVHD. Due to their rapid recovery early after allo-HCT and their ability to kill malignant targets without prior exposure, natural killer (NK) cells have been considered one of the main effector cells that mediate early GVL reactions. Conversely, regulatory T ells (Tregs) have proven to be critical in facilitating self-tolerance. Both murine and human studies have demonstrated a significant role for Tregs in the modulation of GVHD after allo-HCT. This article reviews the mechanisms of how these 2 cell types carry out these functions, focusing on the post-allo-HCT period. Surprisingly, relatively few studies have addressed how Tregs and NK cells interact with one another and whether these interactions are antagonistic. Although preclinical studies suggest active cross-talk between NK cells and Tregs, early clinical studies have not shown a detrimental impact of Treg therapy on relapse. Despite this, interruption of tolerogenic signals may enhance the efficacy of NK effector functions. Methods to transiently impair Treg functions and augment NK cell alloreactivity will be discussed.
机译:限制同种异体造血细胞移植(allo-HCT)功效的两个主要并发症是疾病复发和GVHD。由于它们在同种HCT后早期迅速恢复,并且无需事先暴露就可以杀死恶性靶标,因此自然杀伤(NK)细胞被认为是介导早期GVL反应的主要效应细胞之一。相反,事实证明,调节性推论(Tregs)对于促进自我宽容至关重要。小鼠和人体研究均显示,异基因-HCT后Treg在调节GVHD中起重要作用。本文重点介绍al-HCT后时期这两种细胞类型如何实现这些功能的机制。出乎意料的是,相对较少的研究已经探讨了Tregs和NK细胞如何相互作用以及这些相互作用是否具有拮抗作用。尽管临床前研究表明NK细胞与Tregs之间存在活跃的相互作用,但早期的临床研究并未显示Treg治疗对复发具有有害影响。尽管如此,致耐受信号的中断可能会增强NK效应子功能的功效。将讨论暂时破坏Treg功能并增强NK细胞同种异体反应性的方法。

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