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Cellular aging of skeletal muscle: telomerie and free radical evidence that physical-Inactivity is responsible and not age

机译:骨骼肌细胞衰老:端子和自由基证据,即身体不活动是负责任而不是年龄

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Telomeres play an essential role in maintaining chromosomal integrity in the face of physiological stressors. Although the age-related shortening of TL (telomere length) in highly proliferative tissue is predominantly due to the replication process, the mechanism for telomere shortening in skeletal muscle, which is minimally proliferative, is unclear. By studying TL in both the upper and lower limbs of the young, old-mobile and old-immobile subjects and by virtue of the bipedal nature of human locomotion, which declines with age, it may be possible to elucidate the mechanism(s) responsible for cellular aging of skeletal muscle. With this approach, we revealed that TL (~15 kb) in arm skeletal muscle is unaffected by age. In contrast TL fell progressively in the legs across the young (~15 kb), the old mobile (~13 kb) and old immobile (~11 kb) subjects. Interestingly, there was a reciprocal increase in leg muscle free radicals across these groups that was correlated with TL (r = 0.7), with no such relationship in the arm (r = 0.09). Our results document that chronological age does not affect the cellular aging of skeletal muscle, but reveals that physical inactivity, probably mediated by free radicals, has a profound effect upon this process.
机译:端粒在对生理压力源的染色体完整性中起重要作用。尽管在高增殖组织中的TL(端粒长度)的年龄相关缩短是由于复制过程,但是骨骼肌中端粒体缩短的机制尚不清楚。通过在年轻,老移动和老年人和老年人的上肢和下肢研究TL,并且凭借人类运动的BipeDal性质,随着年龄的增长,可能会阐明负责的机制用于骨骼肌的细胞老化。通过这种方法,我们透露,ARM骨骼肌中的TL(〜15 kB)不受年龄的影响。在对比度中,TL逐渐在腿上逐渐下降(〜15 kB),旧的手机(〜13 kB)和旧的固定(〜11 kB)科目。有趣的是,这些基团的腿部肌肉自由基互殖增加与T1(r = 0.7)相关,在臂中没有这种关系(r = 0.09)。我们的结果证明,年龄年龄的年龄不会影响骨骼肌的细胞衰老,但揭示了可能对该方法产生深远影响的物理不活跃。

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