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Clec9a-Mediated Ablation of Conventional Dendritic Cells Suggests a Lymphoid Path to Generating Dendritic Cells In Vivo

机译:Clec9a介导的常规树突细胞的消融表明在体内产生树突细胞的淋巴路径

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摘要

Conventional dendritic cells (cDCs) are versatile activators of immune responses that develop as part of the myeloid lineage downstream of hematopoietic stem cells. We have recently shown that in mice precursors of cDCs, but not of other leukocytes, are marked by expression of DNGR-1/CLEC9A. To genetically deplete DNGR-1-expressing cDC precursors and their progeny, we crossed Clec9a-Cre mice to Rosa-lox-STOP-lox-diphtheria toxin (DTA) mice. These mice develop signs of age-dependent myeloproliferative disease, as has been observed in other DC-deficient mouse models. However, despite efficient depletion of cDC progenitors in these mice, cells with phenotypic characteristics of cDCs populate the spleen. These cells are functionally and transcriptionally similar to cDCs in wild type control mice but show somatic rearrangements of Ig-heavy chain genes, characteristic of lymphoid origin cells. Our studies reveal a previously unappreciated developmental heterogeneity of cDCs and suggest that the lymphoid lineage can generate cells with features of cDCs when myeloid cDC progenitors are impaired.
机译:常规的树突细胞(CDC)是免疫应答的通酯激活剂,其作为造血干细胞下游的骨髓谱系的一部分发展。我们最近表明,在CDC的小鼠前体,但不是其他白细胞,通过DNGR-1 / CLEC9A的表达标记。为了基因上耗尽DNGR-1表达CDC前体及其后代,我们将CLEC9A-CRE小鼠交叉于ROSA-LOX-STOP-LOX-毒药毒素(DTA)小鼠。这些小鼠在其他直流缺乏小鼠模型中观察到,这些小鼠产生了依赖性髓鳞状疾病的迹象。然而,尽管在这些小鼠中有效地耗尽了CDC祖细胞,但CDC的表型特征的细胞填充了脾脏。这些细胞在功能上并与野生型对照小鼠中的CDC相似,但显示IG重链基因的细胞重排,淋巴源细胞的特征。我们的研究揭示了疾病疾病疾病疾病疾病疾病患者的未被覆富的发育异质性,并表明淋巴谱系可以在粘蛋白CDC祖细胞受损时产生具有CDC的特征的细胞。

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