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鉴定具有向常规树突状细胞分化可塑性的 CCR9- 小鼠浆细胞样树突状细胞前体。

Identification of CCR9- murine plasmacytoid DC precursors with plasticity to differentiate into conventional DCs.

机构信息

II Medical Department, Klinikum rechts der Isar, Technical University Munich, Trogerstrasse 32/1.04, Munich, Germany.

出版信息

Blood. 2011 Jun 16;117(24):6562-70. doi: 10.1182/blood-2010-12-326678. Epub 2011 Apr 20.

Abstract

Whereas the final differentiation of conventional dendritic cells (CDCs) from committed precursors occurs locally in secondary lymphoid or peripheral tissues, plasmacytoid dendritic cells (PDCs) are thought to fully develop in the bone marrow from common DC progenitors before migrating to the periphery. In our study, we define, for the first time, a subpopulation of CCR9(-) major histocompatibility complex class II(low) PDCs in murine bone marrow, which express E2-2 and are immediate precursors of CCR9(+) fully differentiated PDCs. However, CCR9(-) PDCs have the plasticity to acquire the phenotype and function of CD11b(+) CD8α(-) major histocompatibility complex class II(high) CDC-like cells under the influence of soluble factors produced by intestinal epithelial cells or recombinant GM-CSF. This deviation from the PDC lineage commitment is regulated on the level of transcription factors reflected by down-regulation of E2-2 and up-regulation of ID2, PU.1, and BATF3. Thus, CCR9(-) PDCs are immediate PDC precursors that can be reprogrammed to differentiate into CDC-like cells with higher antigen-presenting and cytokine-producing capacity under the influence of the local tissue microenvironment.

摘要

虽然传统树突状细胞(conventional dendritic cells,CDCs)从定向前体细胞在次级淋巴或外周组织中局部最终分化,但浆细胞样树突状细胞(plasmacytoid dendritic cells,PDCs)被认为是从普通树突状细胞前体在骨髓中完全发育,然后迁移到外周。在我们的研究中,我们首次在鼠骨髓中定义了一个 CCR9(-) 主要组织相容性复合体 II(low) PDC 亚群,该亚群表达 E2-2,是 CCR9(+) 完全分化 PDC 的直接前体。然而,在肠上皮细胞或重组 GM-CSF 产生的可溶性因子的影响下,CCR9(-)PDC 具有获得 CD11b(+) CD8α(-) 主要组织相容性复合体 II(high) 类似 CDC 细胞表型和功能的可塑性。这种偏离 PDC 谱系的分化是由转录因子的调节控制的,表现为 E2-2 的下调和 ID2、PU.1 和 BATF3 的上调。因此,CCR9(-)PDC 是直接的 PDC 前体,在局部组织微环境的影响下,可以被重新编程为分化为具有更高抗原呈递和细胞因子产生能力的类似 CDC 细胞。

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