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PGC-1α/β induced expression partially compensates for respiratory chain defects in cells from patients with mitochondrial disorders

机译:PGC-1α/β诱导的表达可部分补偿线粒体疾病患者细胞的呼吸链缺陷

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Members of the peroxisome proliferator-activated receptor γ coactivator (PGC) family are potent inducers of mitochondrial biogenesis. We have tested the potential effect of increased mitochondrial biogenesis in cells derived from patients harboring oxidative phosphorylation defects due to either nuclear or mitochondrial DNA mutations. We found that the PGC-1α and/or PGC-1β expression improved mitochondrial respiration in cells harboring a complex III or IV deficiency as well as in transmitochondrial cybrids harboring mitochondrial encephalomyopathy lactic acidosis and stroke A3243G tRNA(Leu)UUR gene mutation. The respiratory function improvement was found to be associated with increased levels of mitochondrial components per cell, although this increase was not homogeneous. These results reinforce the concept that increased mitochondrial biogenesis is a promising venue for the treatment of mitochondrial diseases.
机译:过氧化物酶体增殖物激活受体γ共激活物(PGC)家族的成员是线粒体生物发生的有效诱导剂。我们已经测试了由由于核或线粒体DNA突变而具有氧化磷酸化缺陷的患者来源的细胞中增加的线粒体生物发生的潜在作用。我们发现PGC-1α和/或PGC-1β的表达改善了具有复杂的III或IV缺陷的细胞以及具有线粒体脑病乳酸性酸中毒和中风的A3243G tRNA (Leu)UUR sup>基因突变。呼吸功能的改善与每个细胞的线粒体成分水平增加有关,尽管这种增加并不均匀。这些结果强化了以下观念:线粒体生物发生增加是治疗线粒体疾病的有前途的场所。

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