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Localized SCF and IGF-1 secretion enhances erythropoiesis in the spleen of murine embryos

机译:局部SCF和IGF-1分泌增强鼠胚胎脾中的红细胞生成

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Fetal spleen is a major hematopoietic site prior to initiation of bone marrow hematopoiesis. Morphologic analysis suggested erythropoietic activity in fetal spleen, but it remained unclear how erythropoiesis was regulated. To address this question, we performed flow cytometric analysis and observed that the number of spleen erythroid cells increased 18.6-fold from 16.5 to 19.5 days post-coitum (dpc). Among erythropoietic cytokines, SCF and IGF-1 were primarily expressed in hematopoietic, endothelial and mesenchymal-like fetal spleen cells. Cultures treated with SCF and/or IGF-1R inhibitors showed significantly decreased CD45?c-Kit?CD71+/?Ter119+ erythroid cells and downregulated Gata1 , Klf1 and β-major globin expression. Administration of these inhibitors to pregnant mice significantly decreased the number of CD45?c-Kit?CD71+/?Ter119+ cells and downregulated β-major globin gene expression in embryos derived from these mice. We conclude that fetal spleen is a major erythropoietic site where endothelial and mesenchymal-like cells primarily accelerate erythropoietic activity through SCF and IGF-1 secretion.
机译:胎儿脾是骨髓造血开始前的主要造血部位。形态学分析提示胎儿脾脏有促红细胞生成活性,但尚不清楚如何调节促红细胞生成。为了解决这个问题,我们进行了流式细胞仪分析,观察到脾红细胞的数量从冠状动脉术后(dpc)的16.5天增加到19.5天增加了18.6倍。在促红细胞因子中,SCF和IGF-1主要在造血,内皮和间充质样胎儿脾脏细胞中表达。用SCF和/或IGF-1R抑制剂处理的培养物显示CD45?c-Kit?CD71 + /?Ter119 +红细胞显着减少,并且Gata1,Klf1和β-主要球蛋白表达下调。将这些抑制剂施用于怀孕的小鼠可显着减少源自这些小鼠的胚胎中CD45Δc-KitΔCD71+ /ΔTer119+细胞的数量,并下调β-主要球蛋白基因的表达。我们得出的结论是,胎儿脾脏是主要的促红细胞生成部位,内皮细胞和间充质样细胞主要通过SCF和IGF-1分泌促进促红细胞生成活性。

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