Maier D, Farr C L, Poeck B, Alahari A, Vogel M, Fischer S, Kaguni L S, Schneuwly S
Lehrstuhl für Entwicklungsbiologie, Universität Regensburg, Regensburg, Germany D-93040.
Mol Biol Cell. 2001 Apr;12(4):821-30. doi: 10.1091/mbc.12.4.821.
The discovery that several inherited human diseases are caused by mtDNA depletion has led to an increased interest in the replication and maintenance of mtDNA. We have isolated a new mutant in the lopo (low power) gene from Drosophila melanogaster affecting the mitochondrial single-stranded DNA-binding protein (mtSSB), which is one of the key components in mtDNA replication and maintenance. lopo(1) mutants die late in the third instar before completion of metamorphosis because of a failure in cell proliferation. Molecular, histochemical, and physiological experiments show a drastic decrease in mtDNA content that is coupled with the loss of respiration in these mutants. However, the number and morphology of mitochondria are not greatly affected. Immunocytochemical analysis shows that mtSSB is expressed in all tissues but is highly enriched in proliferating tissues and in the developing oocyte. lopo(1) is the first mtSSB mutant in higher eukaryotes, and its analysis demonstrates the essential function of this gene in development, providing an excellent model to study mitochondrial biogenesis in animals.
几种遗传性人类疾病由线粒体DNA(mtDNA)耗竭引起这一发现,引发了人们对mtDNA复制和维持的更多关注。我们从黑腹果蝇中分离出一个lopo(低功率)基因的新突变体,该突变体影响线粒体单链DNA结合蛋白(mtSSB),而mtSSB是mtDNA复制和维持的关键成分之一。lopo(1)突变体在变态完成前的三龄后期死亡,原因是细胞增殖失败。分子、组织化学和生理学实验表明,这些突变体中mtDNA含量急剧下降,并伴随着呼吸作用丧失。然而,线粒体的数量和形态并未受到太大影响。免疫细胞化学分析表明,mtSSB在所有组织中均有表达,但在增殖组织和发育中的卵母细胞中高度富集。lopo(1)是高等真核生物中的首个mtSSB突变体,对其分析证明了该基因在发育中的重要功能,为研究动物线粒体生物发生提供了一个极佳模型。
