成年小鼠非神经组织中 HtrA2/Omi 活性的丧失导致早衰。
Loss of HtrA2/Omi activity in non-neuronal tissues of adult mice causes premature aging.
机构信息
Department of Biochemistry and Molecular Biology, The Kimmel Cancer Center, Thomas Jefferson University, Philadelphia, PA 19107, USA.
出版信息
Cell Death Differ. 2013 Feb;20(2):259-69. doi: 10.1038/cdd.2012.117. Epub 2012 Sep 14.
Abstract
mnd2 mice die prematurely as a result of neurodegeneration 30-40 days after birth due to loss of the enzymatic activity of the mitochondrial quality control protease HtrA2/Omi. Here, we show that transgenic expression of human HtrA2/Omi in the central nervous system of mnd2 mice rescues them from neurodegeneration and prevents their premature death. Interestingly, adult transgenic mnd2 mice develop accelerated aging phenotypes, such as premature weight loss, hair loss, reduced fertility, curvature of the spine, heart enlargement, increased autophagy, and death by 12-17 months of age. These mice also have elevated levels of clonally expanded mitochondrial DNA (mtDNA) deletions in their tissues. Our results provide direct genetic evidence linking mitochondrial protein quality control to mtDNA deletions and aging in mammals.
摘要
mnd2 小鼠由于线粒体质量控制蛋白酶 HtrA2/Omi 的酶活性丧失,在出生后 30-40 天会因神经退行性变而过早死亡。在这里,我们表明,在 mnd2 小鼠的中枢神经系统中转基因表达人 HtrA2/Omi 可挽救其免受神经退行性变并防止其过早死亡。有趣的是,成年转基因 mnd2 小鼠会出现加速衰老表型,例如体重过早减轻、脱发、生育力降低、脊柱弯曲、心脏增大、自噬增加以及在 12-17 个月时死亡。这些小鼠的组织中还存在大量克隆扩增的线粒体 DNA(mtDNA)缺失。我们的研究结果提供了直接的遗传证据,将线粒体蛋白质质量控制与哺乳动物的 mtDNA 缺失和衰老联系起来。
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