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首页> 外文期刊>FEBS Open Bio >Impaired respiratory function in MELAS-induced pluripotent stem cells with high heteroplasmy levels
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Impaired respiratory function in MELAS-induced pluripotent stem cells with high heteroplasmy levels

机译:高异质性水平的MELAS诱导多能干细胞呼吸功能受损

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Mitochondrial diseases are heterogeneous disorders, caused by mitochondrial dysfunction. Mitochondria are not regulated solely by nuclear genomic DNA but by mitochondrial DNA. It is difficult to develop effective therapies for mitochondrial disease because of the lack of mitochondrial disease models. Mitochondrial myopathy, encephalomyopathy, lactic acidosis, and stroke-like episodes (MELAS) is one of the major mitochondrial diseases. The aim of this study was to generate MELAS-specific induced pluripotent stem cells (iPSCs) and to demonstrate that MELAS-iPSCs can be models for mitochondrial disease. We successfully established iPSCs from the primary MELAS-fibroblasts carrying 77.7% of m.3243A>G heteroplasmy. MELAS-iPSC lines ranged from 3.6% to 99.4% of m.3243A>G heteroplasmy levels. The enzymatic activities of mitochondrial respiratory complexes indicated that MELAS-iPSC-derived fibroblasts with high heteroplasmy levels showed a deficiency of complex I activity but MELAS-iPSC-derived fibroblasts with low heteroplasmy levels showed normal complex I activity. Our data indicate that MELAS-iPSCs can be models for MELAS but we should carefully select MELAS-iPSCs with appropriate heteroplasmy levels and respiratory functions for mitochondrial disease modeling.
机译:线粒体疾病是由线粒体功能障碍引起的异质性疾病。线粒体不仅受核基因组DNA的调控,还受线粒体DNA的调控。由于缺乏线粒体疾病模型,难以开发有效的线粒体疾病治疗方法。线粒体肌病,脑病,乳酸性酸中毒和中风样发作(MELAS)是主要的线粒体疾病之一。这项研究的目的是生成MELAS特异性诱导多能干细胞(iPSC),并证明MELAS-iPSC可以作为线粒体疾病的模型。我们成功地从携带ME.3243A> G异质性的77.7%的原始MELAS成纤维细胞中建立了iPSC。 MELAS-iPSC品系占m.3243A> G杂种水平的3.6%至99.4%。线粒体呼吸道复合物的酶活性表明,异质水平高的MELAS-iPSC来源的成纤维细胞缺乏复合物I活性,而异质水平低的MELAS-iPSC来源的成纤维细胞显示出复杂的I酶活性。我们的数据表明,MELAS-iPSC可以作为MELAS的模型,但我们应该仔细选择具有适当异质性水平和呼吸功能的MELAS-iPSC,用于线粒体疾病建模。

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