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脑脊液影响髓样树突状细胞的表型和功能。

Cerebrospinal fluid affects phenotype and functions of myeloid dendritic cells.

作者信息

Pashenkov M, Söderström M, Huang Y-M, Link H

机构信息

Division of Neurology, Neuroimmunology Unit, Huddinge University, Stockholm, Sweden.

出版信息

Clin Exp Immunol. 2002 May;128(2):379-87. doi: 10.1046/j.1365-2249.2002.01850.x.

Abstract

Myeloid (CD11c+) dendritic cells (DC) are present in cerebrospinal fluid (CSF), as well as in the meninges and choroid plexus. Functional studies of these DC are hindered or impossible. To obviate this problem, we investigated the effects of CSF supernatants from patients with non-inflammatory neurological diseases (NIND), multiple sclerosis (MS), bacterial meningitis (BM) and Lyme meningoencephalitis (LM) on immature monocyte-derived DC (moDC) from healthy donors. CSF supernatants caused maturation of moDC (MS > LM > NIND > BM), as reflected by a decrease in CD1a, and an increase in HLA-DR, CD80 and CD86 expression. The maturation effect of MS CSF and LM CSF could be blocked by anti-TNF-alpha MoAb or recombinant human IL-10. moDC cultured with BM CSF either remained immature or turned into CD14+ macrophage-like cells and were relatively inefficient at inducing T cell responses in vitro. In contrast, moDC cultured with LM CSF induced strong Th1 responses. Both BM CSF and LM CSF contained IFN-gamma, a cytokine that augments IL-12 production by moDC and hence should confer an ability to induce a Th1 response. However, BM CSF also contained high levels of IL-10, which could antagonize the effects of IFN-gamma on moDC. moDC cultured with MS CSF induced a higher production of IFN-gamma from T cells compared to moDC cultured with NIND CSF or BM CSF. In summary, soluble factors present in the CSF may influence the phenotype and functions of meningeal, choroid plexus and CSF DC which, in turn, may have an impact on the character of intrathecal T cell responses.

摘要

髓样(CD11c +)树突状细胞(DC)存在于脑脊液(CSF)以及脑膜和脉络丛中。对这些DC的功能研究受到阻碍或无法进行。为了解决这个问题,我们研究了非炎性神经系统疾病(NIND)、多发性硬化症(MS)、细菌性脑膜炎(BM)和莱姆脑膜脑炎(LM)患者的脑脊液上清液对健康供体来源的未成熟单核细胞衍生DC(moDC)的影响。脑脊液上清液导致moDC成熟(MS>LM>NIND>BM),表现为CD1a减少,HLA - DR、CD80和CD86表达增加。MS脑脊液和LM脑脊液的成熟作用可被抗TNF -α单克隆抗体或重组人IL - 10阻断。用BM脑脊液培养的moDC要么保持未成熟状态,要么转变为CD14 +巨噬细胞样细胞,并且在体外诱导T细胞反应方面相对效率较低。相比之下,用LM脑脊液培养的moDC诱导强烈的Th1反应。BM脑脊液和LM脑脊液都含有IFN -γ,一种可增强moDC产生IL - 12的细胞因子,因此应该赋予诱导Th1反应的能力。然而,BM脑脊液也含有高水平的IL - 10,它可以拮抗IFN -γ对moDC的作用。与用NIND脑脊液或BM脑脊液培养的moDC相比,用MS脑脊液培养的moDC诱导T细胞产生更高水平的IFN -γ。总之,脑脊液中存在的可溶性因子可能影响脑膜、脉络丛和脑脊液DC的表型和功能,进而可能对鞘内T细胞反应的特征产生影响。

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