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小鼠胰腺中的巨噬细胞及其在体外胎儿内分泌发育中的作用。

Macrophages in the murine pancreas and their involvement in fetal endocrine development in vitro.

作者信息

Geutskens S B, Otonkoski T, Pulkkinen M-A, Drexhage H A, Leenen P J M

机构信息

Department of Immunology, Erasmus MC, Rotterdam, The Netherlands.

出版信息

J Leukoc Biol. 2005 Oct;78(4):845-52. doi: 10.1189/jlb.1004624. Epub 2005 Jul 21.

DOI:10.1189/jlb.1004624
PMID:16037409
Abstract

Macrophages are a heterogeneous population of cells that belong to the mononuclear phagocyte system. They play an important role in tissue homeostasis and remodeling and are also potent immune regulators. Pancreatic macrophages are critically involved in the development and pathogenesis of autoimmune diabetes. To elucidate the ontogeny of pancreatic macrophages, we characterized in this study the macrophages present in the adult and developing fetal pancreas of normal mice. We additionally examined the presence of local macrophage precursors and the involvement of macrophages in the growth of endocrine tissue in the fetal pancreas. We identified two phenotypically distinct macrophage subsets in the adult pancreas. The majority of macrophages was CD45(+)ER-MP23(+)MOMA-1(+). Under noninflammatory conditions, only a minority ( approximately 5%) of the pancreatic macrophages additionally expressed the macrophage marker F4/80. In contrast, in the fetal pancreas, phenotypically, mature macrophages were identified exclusively by their expression of F4/80 and lacked detectable staining with ER-MP23 and MOMA-1 antibodies. In fetal pancreas organ cultures, we could show that macrophages develop from pre-existing precursors, which are present in the fetal pancreas at embryonic age 12.5. Moreover, the number of macrophages increased significantly when macrophage-colony stimulating factor was added to these cultures. It is important that this increase of F4/80-positive cells was paralleled by an increase in the number of insulin-producing cells, suggesting that macrophages support the growth of these endocrine cells.

摘要

巨噬细胞是属于单核吞噬细胞系统的异质性细胞群体。它们在组织稳态和重塑中发挥重要作用,也是强大的免疫调节因子。胰腺巨噬细胞在自身免疫性糖尿病的发生发展和发病机制中起关键作用。为了阐明胰腺巨噬细胞的个体发生,我们在本研究中对正常小鼠成年和发育中的胎儿胰腺中的巨噬细胞进行了特征描述。我们还检测了局部巨噬细胞前体的存在以及巨噬细胞在胎儿胰腺内分泌组织生长中的作用。我们在成年胰腺中鉴定出两个表型不同的巨噬细胞亚群。大多数巨噬细胞为CD45(+)ER-MP23(+)MOMA-1(+)。在非炎症条件下,只有少数(约5%)胰腺巨噬细胞额外表达巨噬细胞标志物F4/80。相比之下,在胎儿胰腺中,从表型上看,成熟巨噬细胞仅通过其F4/80表达来鉴定,并且用ER-MP23和MOMA-1抗体检测不到染色。在胎儿胰腺器官培养中,我们可以证明巨噬细胞由预先存在的前体发育而来,这些前体在胚胎12.5天时存在于胎儿胰腺中。此外,当向这些培养物中添加巨噬细胞集落刺激因子时,巨噬细胞数量显著增加。重要的是,F4/80阳性细胞的这种增加与胰岛素产生细胞数量的增加平行,这表明巨噬细胞支持这些内分泌细胞的生长。

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