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Optimal Versus Realized Trajectories of Physiological Dysregulation in Aging and Their Relation to Sex-Specific Mortality Risk

机译:衰老中生理失调的最佳与实现轨迹及其与性别死亡率风险的关系

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While longitudinal changes in biomarker levels and their impact on health have been characterized for individual markers, little is known about how overall marker profiles may change during aging and affect mortality risk. We implemented the recently developed measure of physiological dysregulation based on the statistical distance of biomarker profiles in the framework of the stochastic process model of aging, using data on blood pressure, heart rate, cholesterol, glucose, hematocrit, body mass index, and mortality in the Framingham original cohort. This allowed us to evaluate how physiological dysregulation is related to different aging-related characteristics such as decline in stress resistance and adaptive capacity (which typically are not observed in the data and thus can be analyzed only indirectly), and, ultimately, to estimate how such dynamic relationships increase mortality risk with age. We found that physiological dysregulation increases with age; that increased dysregulation is associated with increased mortality, and increasingly so with age; and that, in most but not all cases, there is a decreasing ability to return quickly to baseline physiological state with age. We also revealed substantial sex differences in these processes, with women becoming dysregulated more quickly but with men showing a much greater sensitivity to dysregulation in terms of mortality risk.
机译:尽管已针对单个标记物表征了生物标记物水平的纵向变化及其对健康的影响,但人们对整体标记物在衰老过程中如何变化并影响死亡风险知之甚少。我们在年龄随机过程模型的框架内,根据生物标志物分布的统计距离,利用血压,心率,胆固醇,葡萄糖,血细胞比容,体重指数和死亡率等数据,实施了最近开发的生理失调措施。弗雷明汉原始队列。这使我们能够评估生理失调与不同的与衰老相关的特征如何相关,例如抗压力下降和适应能力下降(通常在数据中未观察到,因此只能间接分析),并最终估算出这种动态关系会随着年龄的增长而增加死亡风险。我们发现生理失调随着年龄的增长而增加。失调的增加与死亡率的增加有关,并且随着年龄的增长而增加;而且,在大多数情况下(但不是全部),随着年龄的增长,迅速恢复到基线生理状态的能力正在下降。我们还发现,在这些过程中,性别存在重大差异,女性变得异常失调的速度更快,而男性对死亡风险的失调敏感性更高。

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