首页> 外文期刊>European Journal of Immunology >CXCR3 blockade inhibits T-cell migration into the CNS during EAE and prevents development of adoptively transferred, but not actively induced, disease.
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CXCR3 blockade inhibits T-cell migration into the CNS during EAE and prevents development of adoptively transferred, but not actively induced, disease.

机译:CXCR3封锁抑制t细胞迁移到中枢神经系统,防止在实验性自身免疫性脑脊髓炎的发展过继转移,但不积极诱导,疾病。

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摘要

Autoreactive T-cell infiltration into the CNS is critical in MS and EAE. The chemokine receptor CXCR3 and its ligands are implicated in MS and mouse EAE, but the contribution of CXCR3 to T-cell migration into the inflamed CNS remains controversial. During active disease in a rat EAE model, blood T-cell, spleen T-cell and T lymphoblast migration into the CNS was inhibited by a CXCR3 blocking mAb by, 30-70%, approximately 75% and 50-80%, respectively. However, CXCR3 blockade after active immunization did not inhibit EAE, did not alter total T-cell accumulation in the CNS and did not affect Treg accumulation or the presence of cells producing IFN-gamma or IL-17. Conversely, CXCR3 blockade during EAE induced by adoptive transfer of myelin basic protein-activated T cells delayed disease onset, shortened its duration and reduced disease severity. Moreover, CXCR3 blockade inhibited leukocyte infiltration of the CNS>95%, virtually abolishing infiltration of transferred T cells. Thus, CXCR3 plays a major role in T-cell migration to the CNS and can be critical for encephalitogenic T-cell migration into the CNS to induce disease, but CXCR3-independent recruitment can also produce EAE.
机译:Autoreactive t细胞渗透进入中枢神经系统MS和运算单元的关键。CXCR3和女士及其配体参与鼠标运算单元,但CXCR3的贡献t细胞迁移到中枢神经系统炎症仍然存在有争议的。模型,血T细胞、脾脏T细胞和T淋巴母细胞迁移到中枢神经系统抑制由CXCR3阻塞马伯,大约30 - 70%分别为75%和50 - 80%。主动免疫接种后没有封锁总t细胞,抑制实验性自身免疫性脑脊髓炎并没有改变在中枢神经系统,不影响Treg积累积累或细胞生产的存在IFN-gamma或IL-17。过继转移引起的髓磷脂在实验性自身免疫性脑脊髓炎基本protein-activated T细胞延迟疾病发病,缩短其持续时间和减少疾病严重性。白细胞浸润的中枢神经系统> 95%,几乎废除的渗透转移T细胞。因此,CXCR3在t细胞中起着重要的作用迁移到中枢神经系统,可以的关键encephalitogenic t细胞迁移到中枢神经系统诱发疾病,但CXCR3-independent招聘也可以产生运算单元。

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