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首页> 外文期刊>Journal of Neuroimmunology: Official Bulletin of the Research Committee on Neuroimmunology of the World Federation of Neurology >Site-specific control of T cell traffic in the brain: T cell entry to brainstem vs. hippocampus after local injection of IFN-gamma.
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Site-specific control of T cell traffic in the brain: T cell entry to brainstem vs. hippocampus after local injection of IFN-gamma.

机译:大脑中T细胞运输的部位特异性控制:局部注射IFN-γ后,T细胞进入脑干与海马区。

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摘要

Although it is known that neurotransmitters and neuropeptides can affect immune function in vitro, less is understood about how the neural environment affects immune function in the brain. Previously, we showed that regulation of parenchymal class II MHC after local injection of IFN-gamma is site-specific. In this companion study, we defined the effect of local IFN-gamma on the entry of class II-restricted T cells to the brain parenchyma. To activate endogenous T cells, adult CDF rats were immunized with a normal neural antigen (MBP). Two weeks later, the proinflammatory cytokine IFN-gamma (100 to 10,000 U/site) was injected stereotaxically into two neurochemically and anatomically distinct sites, the hippocampus (area CAI) and brainstem (nucleus of the solitary tract). Monoclonal R73 was used to detect T cells on cryostat sections. The greatest difference was seen 48 h after 300 U IFN-gamma was injected at each site, when there were several-fold more parenchymal T cells in the brainstem than in the hippocampus. Most parenchymal T cells were CD4+ /class II-restricted. Thus, parenchymal T cell entry and parenchymal class II up-regulation show the same hierarchy (brainstem hippocampus) after local IFN-gamma injection, although T cell entry was more sensitive to the IFN-gamma dose. We suggest that the local regulatory environment contributes to site-specific immune regulation, and discuss implications for the distribution of MS plaques and other aspects of local immune control. Further, in interpreting the many previous studies of cytokine-mediated immune changes in the CNS, the possibility of site-specific differences should be considered.
机译:尽管已知神经递质和神经肽可以在体外影响免疫功能,但对于神经环境如何影响大脑的免疫功能知之甚少。以前,我们表明局部注射IFN-γ后对实质II类MHC的调节是位点特异性的。在这项伴随研究中,我们定义了局部IFN-γ对II类限制性T细胞进入脑实质的影响。为了激活内源性T细胞,用正常的神经抗原(MBP)对成年CDF大鼠进行免疫。两周后,将促炎细胞因子IFN-γ(100至10,000 U /位)立体定位注射到两个神经化学和解剖学上不同的位点,即海马区(CAI区)和脑干(孤立道核)。单克隆R73被用于检测低温恒温器切片上的T细胞。当在每个部位注射300 UIFN-γ后48小时,脑干实质T细胞的数量是海马体数量的几倍时,观察到最大的差异。大多数实质性T细胞是CD4 + / II类限制的。因此,虽然T细胞进入对IFN-γ剂量更敏感,但局部T-细胞进入和实质II类上调在局部IFN-γ注射后显示出相同的等级(脑干海马)。我们建议当地监管环境有助于特定地点的免疫调节,并讨论对MS斑块的分布和本地免疫控制的其他方面的影响。此外,在解释以前许多有关中枢神经系统中细胞因子介导的免疫变化的研究时,应考虑位点特异性差异的可能性。

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