Institute of Molecular Psychiatry, University of Bonn, 53127 Bonn, Germany.
Proc Natl Acad Sci U S A. 2012 Mar 6;109(10):3897-902. doi: 10.1073/pnas.1114153109. Epub 2012 Feb 21.
Dendritic cells (DCs) are pivotal for the development of experimental autoimmune encephalomyelitis (EAE). However, the mechanisms by which they control disease remain to be determined. This study demonstrates that expression of CC chemokine receptor 4 (CCR4) by DCs is required for EAE induction. CCR4(-/-) mice presented enhanced resistance to EAE associated with a reduction in IL-23 and GM-CSF expression in the CNS. Restoring CCR4 on myeloid cells in bone marrow chimeras or intracerebral microinjection of CCR4-competent DCs, but not macrophages, restored EAE in CCR4(-/-) mice, indicating that CCR4(+) DCs are cellular mediators of EAE development. Mechanistically, CCR4(-/-) DCs were less efficient in GM-CSF and IL-23 production and also T(H)-17 maintenance. Intraspinal IL-23 reconstitution restored EAE in CCR4(-/-) mice, whereas intracerebral inoculation using IL-23(-/-) DCs or GM-CSF(-/-) DCs failed to induce disease. Thus, CCR4-dependent GM-CSF production in DCs required for IL-23 release in these cells is a major component in the development of EAE. Our study identified a unique role for CCR4 in regulating DC function in EAE, harboring therapeutic potential for the treatment of CNS autoimmunity by targeting CCR4 on this specific cell type.
树突状细胞 (DCs) 在实验性自身免疫性脑脊髓炎 (EAE) 的发展中起着关键作用。然而,它们控制疾病的机制仍有待确定。本研究表明,DCs 表达 C 型趋化因子受体 4 (CCR4) 是诱导 EAE 的必需条件。CCR4(-/-) 小鼠对 EAE 的易感性增强,与 CNS 中 IL-23 和 GM-CSF 表达减少有关。在骨髓嵌合体中或脑内微注射 CCR4 功能正常的 DC 而不是巨噬细胞恢复 CCR4,可在 CCR4(-/-) 小鼠中恢复 EAE,表明 CCR4(+) DC 是 EAE 发展的细胞介导物。从机制上讲,CCR4(-/-) DC 在 GM-CSF 和 IL-23 产生以及 T(H)-17 维持方面效率较低。脊髓内 IL-23 重建可在 CCR4(-/-) 小鼠中恢复 EAE,而脑内接种 IL-23(-/-) DC 或 GM-CSF(-/-) DC 则不能诱导疾病。因此,CCR4 依赖性 GM-CSF 在这些细胞中释放 IL-23 所需的 DC 中产生,是 EAE 发展的一个主要组成部分。我们的研究确定了 CCR4 在调节 EAE 中 DC 功能方面的独特作用,通过针对这种特定细胞类型的 CCR4 进行靶向治疗,为治疗中枢神经系统自身免疫提供了治疗潜力。
