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Early CD30 signaling is critical for adoptively transferred CD4+CD25+ regulatory T cells in prevention of acute graft-versus-host disease

机译:早期CD30信号传导对于过继转移CD4 + CD25 +调节性T细胞在预防急性移植物抗宿主病中至关重要

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摘要

Murine CD4+CD25+ regulatory T cells (Treg cells) reduce acute graft-versus-host disease (aGvHD). However, surface molecules critical for suppression are unclear. Deficiency of CD30 (CD30−/−) leads to impaired thymic negative selection and augmented T-cell autoreactivity. Therefore, we investigated the role of CD30 signaling in Treg-cell function during aGvHD. Treg cells derived from CD30−/− animals were significantly less effective in preventing aGvHD lethality. Early blockade of the CD30/CD153 pathway with a neutralizing anti-CD153 mAb reduced Treg-mediated protection from proinflammatory cytokine accumulation and donor-type T-cell apoptosis. In vivo bioluminescence imaging demonstrated intact homing but reduced expansion of luciferase-expressing Treg cells when CD153 was blocked during the early phase after adoptive transfer. CD30 surface expression on Treg cells increased with alloantigen exposure, and CD153 expression on recipient-type dendritic cells increased in the presence of a proinflammatory environment. These data demonstrate that early CD30 signaling is critical for Treg-mediated aGvHD protection after major MHC-mismatch bone marrow transplantation.
机译:鼠CD4 + CD25 +调节性T细胞(Treg细胞)可减轻急性移植物抗宿主病(aGvHD)。然而,对于抑制至关重要的表面分子尚不清楚。 CD30(CD30-/-)缺乏会导致胸腺阴性选择受损和T细胞自身反应性增强。因此,我们调查了aGvHD期间CD30信号在Treg细胞功能中的作用。源自CD30-/-动物的Treg细胞在预防aGvHD致死性方面的效力明显较低。用中和性抗CD153 mAb早期阻断CD30 / CD153途径可降低Treg介导的对促炎性细胞因子蓄积和供体型T细胞凋亡的保护作用。体内生物发光成像显示完整的归巢,但在过继转移后的早期阶段阻断CD153时,表达荧光素酶的Treg细胞的扩增减少。 Treg细胞上的CD30表面表达随同种抗原暴露而增加,而在前炎症环境下,受体型树突状细胞上的CD153表达增加。这些数据表明,早期的CD30信号传导对于大型MHC不匹配的骨髓移植后Treg介导的aGvHD保护至关重要。

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