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Involvement of IL-2R beta(+) T cells in graft-versus-host disease of the liver and intestine across mutant MHC class I or class II barrier

机译:IL-2R beta(+)T细胞跨突变的MHC I类或II类障碍物参与肝脏和肠道移植物抗宿主病

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摘要

MHC class I mutant B6.C-H-2(bm1) (bm1) mice or MHC class II mutant B6.C-H-2(bm12) (bm12) were sublethally irradiated and received bone marrow (BM) cells from B6 or Thy1.1(+) B10 mice. Most T cells in the liver, spleen and intestine were replaced by donor derived IL-2R beta(+) CD8(+) cells in bm1 mice, while both donor IL-2R beta(+) CD4(+) cells and host T cells were present in bm12 mice 2 weeks after BM transplantation. alpha IEL chain(+) cells and gamma delta T cells decreased in the intestine in bm1 mice, while host gamma delta T cells increased in the intestine of bm12 mice. In bm1 mice, infiltration of leukocytes was observed in the liver sinusoids and portal area. In bm12 mice, Leukocyte infiltration occurred around bile duct and submucosal area of the large intestine. Although most irradiated bm1 or bm12 mice that received lymph node cells alone died within 10 days, mice injected with BM cells and lymph node MNC surivived and expansion of IL-2R beta(+) T cells was less obvious. These results suggest that activated donor IL-2R beta(+) T cells are effecters for graft-versus-host disease across mutant MHC, and BM cells are needed for host survival and suppression of activated donor T cells. [References: 26]
机译:对MHC I类突变体B6.CH-2(bm1)(bm1)小鼠或MHC II类突变体B6.CH-2(bm12)(bm12)进行亚致死性照射,并从B6或Thy1.1( +)B10小鼠。肝脏,脾脏和肠道中的大多数T细胞被bm1小鼠中的供体来源的IL-2R beta(+)CD8(+)细胞替代,而供体IL-2R beta(+)CD4(+)细胞和宿主T细胞BM移植后2周,它们出现在bm12小鼠中。 bm1小鼠肠道中的αIEL链(+)细胞和γδT细胞减少,而bm12小鼠肠中的宿主γδT细胞增加。在bm1小鼠中,在肝窦和门静脉区域观察到白细胞浸润。在bm12小鼠中,白细胞浸润发生在大肠的胆管和粘膜下区域附近。尽管大多数仅接受淋巴结细胞照射的受照射的bm1或bm12小鼠在10天内死亡,但注射BM细胞和淋巴结MNC的小鼠却存活下来,IL-2R beta(+)T细胞的扩张并不明显。这些结果表明,活化的供体IL-2Rβ(+)T细胞是跨突变MHC的移植物抗宿主疾病的效应物,而BM细胞对于宿主存活和活化供体T细胞的抑制是必需的。 [参考:26]

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