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Glucose Induces Glonal Selection and Reversible Dinucleotide Repeat Expansion in Mesangial Cells Isolated from Glomerulosclerosis-Prone Mice

机译:葡萄糖诱导从肾小球硬化症-克隆小鼠分离的系膜细胞中的肾小球选择和可逆二核苷酸重复扩增。

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Clonal selection has been proposed as a pathogenetic mechanism in various chronic diseases, such as sclero-derma, hypertension, pulmonary fibrosis, interstitial fibrosis of the kidney, atherosclerosis, and uterine leiomyomatosis. We previously found that mesangial cells from ROP mice prone to develop glomerulosclero-sis changed their phenotype in response to high glucose concentrations. Here, we investigate whether clonal selection might contribute to this phenotype change. We found that in ROP mice at least two distinct mesangial cell clones exist. They are characterized by a different length of the d(CA) repeat in the MMP-9 promoter and exhibit a significantly different gene expression profile. Exposure of ROP mesangial cells to 25 mmol/l glucose for 35 days induces both clonal selection and reversible dinucleotide repeat expansion. None of these findings were present in mesangial cells isolated from C57BL/6 mice, which are not sclerosis-prone. We conclude that mesangial cell michrochimerism may be a marker for the susceptibility to glomerulosclerosis, that dinucleotide repeat expansion may be a novel mechanism for glucose-induced changes in gene expression, and that clonal selection may partially explain the change in mesangial cell phenotype in diabetes.
机译:已经提出克隆选择作为各种慢性疾病的发病机制,例如硬皮病,高血压,肺纤维化,肾间质纤维化,动脉粥样硬化和子宫平滑肌瘤。我们以前发现,来自ROP小鼠的肾小球系膜细胞易于发生肾小球硬化症,从而改变了其表型以响应高葡萄糖浓度。在这里,我们调查克隆选择是否可能有助于这种表型的变化。我们发现在ROP小鼠中至少存在两个不同的系膜细胞克隆。它们的特征是MMP-9启动子中d(CA)重复序列的长度不同,并且显示出明显不同的基因表达谱。将ROP系膜细胞暴露于25 mmol / l葡萄糖中35天可诱导克隆选择和可逆二核苷酸重复扩增。从C57BL / 6小鼠分离的肾小球系膜细胞中没有这些发现,它们不容易发生硬化。我们得出的结论是,肾小球系膜细胞嵌合体可能是肾小球硬化易感性的标志,二核苷酸重复扩增可能是葡萄糖诱导基因表达变化的新机制,而克隆选择可能部分解释了糖尿病中肾小球膜细胞表型的变化。

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