Notch2 受体信号控制脾脏和肠道中树突状细胞的功能分化。
Notch2 receptor signaling controls functional differentiation of dendritic cells in the spleen and intestine.
机构信息
Department of Microbiology and Immunology, Columbia University Medical Center, New York, NY 10032, USA.
出版信息
Immunity. 2011 Nov 23;35(5):780-91. doi: 10.1016/j.immuni.2011.08.013. Epub 2011 Oct 20.
Abstract
Dendritic cells (DCs) in tissues and lymphoid organs comprise distinct functional subsets that differentiate in situ from circulating progenitors. Tissue-specific signals that regulate DC subset differentiation are poorly understood. We report that DC-specific deletion of the Notch2 receptor caused a reduction of DC populations in the spleen. Within the splenic CD11b(+) DC subset, Notch signaling blockade ablated a distinct population marked by high expression of the adhesion molecule Esam. The Notch-dependent Esam(hi) DC subset required lymphotoxin beta receptor signaling, proliferated in situ, and facilitated CD4(+) T cell priming. The Notch-independent Esam(lo) DCs expressed monocyte-related genes and showed superior cytokine responses. In addition, Notch2 deletion led to the loss of CD11b(+)CD103(+) DCs in the intestinal lamina propria and to a corresponding decrease of IL-17-producing CD4(+) T cells in the intestine. Thus, Notch2 is a common differentiation signal for T cell-priming CD11b(+) DC subsets in the spleen and intestine.
摘要
组织和淋巴器官中的树突状细胞 (DC) 包含不同的功能亚群,这些亚群在循环祖细胞中就地分化而来。调节 DC 亚群分化的组织特异性信号尚不清楚。我们报告称, Notch2 受体在 DC 中的特异性缺失导致脾脏中 DC 群体减少。在脾脏 CD11b(+) DC 亚群中,Notch 信号阻断消除了一个以粘附分子 Esam 高表达为特征的独特群体。Notch 依赖性 Esam(hi) DC 亚群需要淋巴毒素β受体信号,在原位增殖,并促进 CD4(+) T 细胞的初始激活。Notch 非依赖性 Esam(lo) DC 表达单核细胞相关基因,并表现出优越的细胞因子反应。此外,Notch2 缺失导致肠道固有层中 CD11b(+)CD103(+) DC 的丧失,以及肠道中 IL-17 产生的 CD4(+) T 细胞相应减少。因此,Notch2 是脾脏和肠道中用于初始激活 CD4(+) T 细胞的 CD11b(+) DC 亚群的共同分化信号。
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