由于氧化应激和其他因素,人类卵泡老化加速的数学模型

A M Portillo;C Peláez
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引用次数: 3

摘要

由于复制机制无法复制染色体的末端,端粒逐渐缩短。此外,其他因素,如高水平的氧化(自由基或活性氧(ROS)),如由于累积的压力,炎症或烟草烟雾,加速端粒缩短。在人类中,端粒在出生时的平均长度约为10-15 kb,端粒以每年70 bp的速度缩短。然而,当细胞暴露于ROS中时,端粒磨损发生的速度更快,产生了不同长度百分位数的各种端粒大小分布,这与年龄所期望的不同。在这项工作中,细胞的世代年龄与其端粒长度(TL)有关,从允许复制的最大端粒长度到最小端粒长度。为了研究衰老颗粒细胞在人卵泡中从卵泡前到排卵前大小的积累,提出了端粒加速缩短的不同程度的数学模型,该模型除了反映细胞分裂后端粒缩短的作用外,还反映了ROS的作用。在TL比平均TL短的细胞,端粒酶活性低,端粒缩短加速的情况下,数学模型预测了排卵前卵泡的衰老结果。该模型为老年妇女的卵母细胞所观察到的情况提供了一个合理的解释,这些卵母细胞暴露于ROS的时间较长,体外受精后的结果较差。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
Mathematical modelling of ageing acceleration of the human follicle due to oxidative stress and other factors
There is a gradual telomere shortening due to the inability of the replication machinery to copy the very ends of chromosomes. Additionally, other factors such as high levels of oxidation (free radicals or reactive oxygen species (ROS)), e.g. due to cumulated stress, inflammation or tobacco smoke, accelerate telomere shortening. In humans, the average telomere length is about 10–15 kb at birth and telomeres shorten at a pace of 70 bp per year. However, when cells are exposed to ROS, telomere attrition happens at a faster pace, generating a wide variety of telomere size distribution in different length percentiles, which are different to what is expected just by age. In this work, the generational age of a cell is associated with its telomere length (TL), from certain maximum to the minimal TL that allows replication. In order to study the accumulation of aged granulosa cells in human follicles, from preantral to preovulatory size, a mathematical model is proposed, regarding different degrees of accelerated telomere shortening, which reflect the action of ROS in addition to the telomere shortening that happens after cell division. In cases of cells with TL shorter than cells with average TL, with low telomerase activity and accelerated telomere shortening, the mathematical model predicts an aged outcome in preovulatory follicles. The model provides a plausible explanation for what has been observed in oocytes from older women, which have been exposed to ROS for a longer period of time and have bad outcomes after in vitro fertilization.
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