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Differentially expressed genes in a porcine adult hepatic stem-like cell line and their expression in developing and regenerating liver

机译:猪成年肝干样细胞系中差异表达的基因及其在肝脏发育和再生中的表达

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To identify differentially expressed genes in adult hepatic stem cells, we performed suppression-subtractive hybridization (SSH) between adult porcine hepatic stem-like cells (HSLCs) and hepatocytes, and the expression of selected genes was assessed in porcine fetal livers and regenerating liver in an 80% hepatectomy model. SSH and subsequent differential screening selected 39 clones that were expressed differentially in HSLCs, including six known genes, 10 unknown genes, one unidentified gene and some chimeric fragments. Four of these genes showed significantly higher expression in HSLCs than in mature hepatocytes: anti-leukoproteinase, matrix Gla protein, amyloid-β precursor protein (APP) and dickkopf-3 (DKK-3). Among them, the mRNA expression of APP and DKK-3 was significantly higher in fifth GW fetal liver than in seventh and thirteenth GW fetal and adult livers, unlike the expression patterns of α-fetoprotein (AFP) or albumin. These mRNAs were detected in the parenchyma of fifth GW fetal liver, whereas in normal adult liver possible expression was limited to the periportal area. On the other hand, immunohistochemistry, Masson's trichrome staining and silver impregnation demonstrated APP and DKK-3 proteins in fifth GW fetal liver in which intralobular bile ducts and hepatic plates had not completely developed. DKK-3 and AFP mRNAs were upregulated on the seventh day (7D) after 80% hepatectomy. In the liver tissue, DKK-3 and AFP proteins were detected in mesenchymal cells in the periportal area and parenchyma, respectively. These data for DKK-3 expression in adult livers suggest the possible presence of adult HSLCs in the periportal area. The pattern of histological staining suggested that 7D liver was in the process of regeneration, showing a character similar to the fifth GW fetal liver. It is speculated that DKK-3 is upregulated in immature and developing livers, and has possible involvement in hepatic differentiation and liver regeneration.
机译:为了鉴定成年肝干细胞中差异表达的基因,我们在成年猪肝干样细胞(HSLC)和肝细胞之间进行了抑制-扣除杂交(SSH),并评估了猪胎肝和再生肝中所选基因的表达。 80%的肝切除模型。 SSH和随后的差异筛选选择了在HSLC中差异表达的39个克隆,包括6个已知基因,10个未知基因,1个未鉴定基因和一些嵌合片段。这些基因中的四个基因在HSLC中显示出比在成熟肝细胞中显着更高的表达:抗白蛋白酶,基质Gla蛋白,淀粉样β前体蛋白(APP)和dickkopf-3(DKK-3)。其中,与α-甲胎蛋白(AFP)或白蛋白的表达模式不同,第五代GW胎儿肝脏中APP和DKK-3的mRNA表达显着高于第七代和第十三种GW胎儿和成年肝脏。在第五代GW胎儿肝脏的实质中检测到了这些mRNA,而在正常的成年肝脏中,可能的表达局限于门周围区域。另一方面,免疫组化,Masson的三色染色和银浸渍显示了第五代GW胎儿肝脏中的APP和DKK-3蛋白,其中小叶内胆管和肝板尚未完全发育。肝切除80%后的第七天(7D)DKK-3和AFP mRNA上调。在肝组织中,分别在门静脉区和实质中的间充质细胞中检测到DKK-3和AFP蛋白。这些DKK-3在成年肝脏中表达的数据表明,在口周区域可能存在成年HSLC。组织学染色的模式表明7D肝脏处于再生过程中,表现出类似于第五代GW胎儿肝脏的特征。据推测,DKK-3在未成熟和发育中的肝脏中被上调,并且可能参与肝分化和肝脏再生。

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