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首页> 外文期刊>Blood: The Journal of the American Society of Hematology >Tolerogenic interactions between CD8(+) dendritic cells and NKT cells prevent rejection of bone marrow and organ grafts
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Tolerogenic interactions between CD8(+) dendritic cells and NKT cells prevent rejection of bone marrow and organ grafts

机译:CD8(+)树突细胞和NKT细胞之间的耐受性相互作用防止骨髓和器官移植物的排斥

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The combination of total lymphoid irradiation and anti-T-cell antibodies safely induces immune tolerance to combined hematopoietic cell and organ allografts in humans. Our mouse model required host natural killer T (NKT) cells to induce tolerance. Because NKT cells normally depend on signals from CD8(+) dendritic cells (DCs) for their activation, we used the mouse model to test the hypothesis that, after lymphoid irradiation, host CD8(+) DCs play a requisite role in tolerance induction through interactions with NKT cells. Selective deficiency of either CD8(+) DCs or NKT cells abrogated chimerism and organ graft acceptance. After radiation, the CD8(+) DCs increased expression of surface molecules required for NKT and apoptotic cell interactions and developed suppressive immune functions, including production of indoleamine 2,3- deoxygenase. Injection of naive mice with apoptotic spleen cells generated by irradiation led to DC changes similar to those induced by lymphoid radiation, suggesting that apoptotic body ingestion by CD8(+) DCs initiates tolerance induction. Tolerogenic CD8(+) DCs induced the development of tolerogenic NKT cells with a marked T helper 2 cell bias that, in turn, regulated the differentiation of the DCs and suppressed rejection of the transplants. Thus, reciprocal interactions between CD8(+) DCs and invariant NKT cells are required for tolerance induction in this system that was translated into a successful clinical protocol.
机译:总淋巴辐射和抗T细胞抗体的组合安全地诱导人类中造血细胞和器官同种异体移植物的免疫耐受性。我们的小鼠模型需要宿主自然杀手T(NKT)细胞来引起耐受性。因为NKT细胞通常取决于来自CD8(+)树突细胞(DCS)的信号进行激活,所以我们使用小鼠模型来测试假设,在淋巴辐射后,宿主CD8(+)DCS在公差诱导中发挥了必要的作用与NKT细胞的相互作用。选择性缺乏CD8(+)DCS或NKT细胞废旧和器官移植物接受。辐射后,CD8(+)DCS增加了NKT和凋亡细胞相互作用所需的表面分子的表达,并产生抑制免疫功能,包括吲哚胺2,3-脱氧酶的产生。用辐射产生的凋亡脾细胞注射幼稚小鼠导致DC变化与淋巴辐射诱导的DC变化,表明CD8(+)DCS摄取的凋亡体引发耐受性诱导。耐受性CD8(+)DCS诱导具有标记的T辅助2细胞偏差的耐受性NKT细胞的发育,又调节DCS的分化并抑制移植物的抑制。因此,该系统中的该系统中的耐受性诱导需要CD8(+)DC和不变NKT细胞之间的互核相互作用,该耐受性被翻译成成功的临床方案。

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