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首页> 外文期刊>The Journal of Immunology: Official Journal of the American Association of Immunologists >Early T Cell Activation Metrics Predict Graft-versus-Host Disease in a Humanized Mouse Model of Hematopoietic Stem Cell Transplantation
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Early T Cell Activation Metrics Predict Graft-versus-Host Disease in a Humanized Mouse Model of Hematopoietic Stem Cell Transplantation

机译:早期T细胞活化度量预测造血干细胞移植的人源化小鼠模型中的移植物与宿主病

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摘要

Acute graft-versus-host disease (GVHD) is a frequent complication of hematopoietic transplantation, yet patient risk stratification remains difficult, and prognostic biomarkers to guide early clinical interventions are lacking. We developed an approach to evaluate the potential of human T cells from hematopoietic grafts to produce GVHD. Nonconditioned NBSGW mice transplanted with titrated doses of human bone marrow developed GVHD that was characterized by widespread lymphocyte infiltration and organ pathology. Interestingly, GVHD was not an inevitable outcome in our system and was influenced by transplant dose, inflammatory status of the host, and type of graft. Mice that went on to develop GVHD showed signs of rapid proliferation in the human T cell population during the first 1-3 wk posttransplant and had elevated human IFN-gamma in plasma that correlated negatively with the expansion of the human hematopoietic compartment. Furthermore, these early T cell activation metrics were predictive of GVHD onset 3-6 wk before phenotypic pathology. These results reveal an early window of susceptibility for pathological T cell activation following hematopoietic transplantation that is not simply determined by transient inflammation resulting from conditioning-associated damage and show that T cell parameters during this window can serve as prognostic biomarkers for risk of later GVHD development.
机译:急性移植物与宿主疾病(GVHD)是造血移植频繁并发症,但患者风险分层仍然困难,预后生物标志物引导缺乏早期临床干预措施。我们开发了一种评估从造血移植物中的人T细胞的潜力以产生GVHD。非典型的NBSGW小鼠移植用滴定剂量的人骨髓显现的GVHD,其特征在于广泛的淋巴细胞浸润和器官病理学。有趣的是,GVHD不是我们系统中不可避免的结果,受移植剂量,宿主炎症状态和移植物的影响。继续开发GVHD的小鼠显示了在前1-3个WK后化合物中人体T细胞群中快速增殖的迹象,并在血浆中升高了人的IFN-Gamma,这些血浆与人造血室的扩张负相关。此外,这些早期的T细胞活化度量是在表型病理学之前的GVHD发作3-6周的预测性。这些结果揭示了在造血移植后的病理T细胞活化易感性的早期窗口,其不仅通过调节相关损伤引起的瞬态炎症确定,并且显示该窗口中的T细胞参数可以作为预后生物标志物,用于以后的GVHD发育风险。

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