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首页> 外文期刊>Liver international : >Physiological variations of stem cell factor and stromal-derived factor-1 in murine models of liver injury and regeneration.
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Physiological variations of stem cell factor and stromal-derived factor-1 in murine models of liver injury and regeneration.

机译:小鼠肝损伤和再生模型中干细胞因子和基质衍生因子-1的生理变化。

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BACKGROUND/AIMS: Stem cell factor (SCF) and stromal-derived factor-1 (SDF-1) regulate the regenerative response to liver injury, possibly through activation of liver progenitor 'oval' cells and recruitment of circulating, marrow-derived progenitors. METHODS: We performed a detailed analysis of SCF, SDF-1 and oval cell proliferation induced by tyrosinaemia, 3,5-diethoxycarbonyl-1,4-dihydrocollidine (DDC) or liver irradiation in mice by ELISA and immunofluorescence. RESULTS: Liver injury in the tyrosinaemia mouse is characterized by a dramatic decline in plasma SCF and absence of oval cell proliferation. In contrast, DDC induces bile duct (BD) and oval cell proliferation, and a modest decline in plasma SCF. Focal liver irradiation increases plasma SCF, but not oval cell density. In normal mouse liver, SCF is localized primarily to Kupffer cells, cholangiocytes and arterial smooth muscle, with little or no expression in hepatocytes. However, SCF appears in hepatocyte nuclei after injury, where its function is unknown. In all three models, SDF-1 is expressed exclusively in BD epithelium, indicating that tissue SDF-1 levels are proportional to the total mass of oval cells and cholangiocytes. However, increased plasma levels of SDF-1 in fumaryl acetoacetate hydroxylase-null mice were not accompanied by oval cell proliferation. CONCLUSION: Changes in SCF and SDF-1 varied with the nature of liver injury and were not directly related to oval cell proliferation.
机译:背景/目的:干细胞因子(SCF)和基质衍生因子1(SDF-1)可能通过激活肝祖卵细胞和募集循环的骨髓祖细胞来调节对肝损伤的再生反应。方法:我们通过ELISA和免疫荧光法对小鼠酪氨酸血症,3,5-二乙氧基羰基-1,4-二氢可力丁(DDC)或肝脏照射诱导的SCF,SDF-1和卵圆细胞增殖进行了详细分析。结果:酪氨酸血症小鼠的肝损伤的特征在于血浆SCF急剧下降,且卵圆细胞没有增殖。相反,DDC诱导胆管(BD)和卵圆形细胞增殖,并导致血浆SCF适度下降。局灶性肝照射可增加血浆SCF,但不能增加卵圆细胞密度。在正常小鼠肝脏中,SCF主要定位于库普弗细胞,胆管细胞和动脉平滑肌,而在肝细胞中几乎没有表达。但是,SCF会在损伤后出现在肝细胞核中,其功能尚不清楚。在所有三个模型中,SDF-1仅在BD上皮中表达,表明组织SDF-1水平与卵圆细胞和胆管细胞的总质量成比例。但是,在富马酰基乙酰乙酸羟化酶无效的小鼠中,血浆SDF-1水平升高并未伴随卵圆形细胞增殖。结论:SCF和SDF-1的变化随肝损伤的性质而变化,与卵圆细胞的增殖没有直接关系。

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