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IGF-1 对健康寿命、病理和寿命具有性别二态、多效和时变的影响。

IGF-1 has sexually dimorphic, pleiotropic, and time-dependent effects on healthspan, pathology, and lifespan.

机构信息

Department of BioMolecular Sciences, University of Mississippi, Oxford, MS, USA.

Reynolds Oklahoma Center on Aging, Department of Geriatric Medicine, University of Oklahoma Health Sciences Center, 975 NE 10th Street, SLY-BRC 1303, Oklahoma City, OK, 73104, USA.

出版信息

Geroscience. 2017 Apr;39(2):129-145. doi: 10.1007/s11357-017-9971-0. Epub 2017 Apr 13.

Abstract

Reduced circulating levels of IGF-1 have been proposed as a conserved anti-aging mechanism that contributes to increased lifespan in diverse experimental models. However, IGF-1 has also been shown to be essential for normal development and the maintenance of tissue function late into the lifespan. These disparate findings suggest that IGF-1 may be a pleiotropic modulator of health and aging, as reductions in IGF-1 may be beneficial for one aspect of aging, but detrimental for another. We postulated that the effects of IGF-1 on tissue health and function in advanced age are dependent on the tissue, the sex of the animal, and the age at which IGF-1 is manipulated. In this study, we examined how alterations in IGF-1 levels at multiple stages of development and aging influence overall lifespan, healthspan, and pathology. Specifically, we investigated the effects of perinatal, post-pubertal, and late-adult onset IGF-1 deficiency using genetic and viral approaches in both male and female igf C57Bl/6 mice. Our results support the concept that IGF-1 levels early during lifespan establish the conditions necessary for subsequent healthspan and pathological changes that contribute to aging. Nevertheless, these changes are specific for each sex and tissue. Importantly, late-life IGF-1 deficiency (a time point relevant for human studies) reduces cancer risk but does not increase lifespan. Overall, our results indicate that the levels of IGF-1 during development influence late-life pathology, suggesting that IGF-1 is a developmental driver of healthspan, pathology, and lifespan.

摘要

循环 IGF-1 水平降低被认为是一种保守的抗衰老机制,它有助于延长不同实验模型的寿命。然而,IGF-1 对于正常发育和组织功能的维持也是必不可少的,直到寿命后期。这些截然不同的发现表明,IGF-1 可能是健康和衰老的多效调节剂,因为 IGF-1 的减少可能对衰老的一个方面有益,但对另一个方面有害。我们假设 IGF-1 对老年组织健康和功能的影响取决于组织、动物的性别以及 IGF-1 被操纵的年龄。在这项研究中,我们研究了在发育和衰老的多个阶段改变 IGF-1 水平如何影响整体寿命、健康寿命和病理。具体来说,我们使用基因和病毒方法研究了围产期、青春期后和成年后期 IGF-1 缺乏对雄性和雌性 igf C57Bl/6 小鼠的影响。我们的结果支持这样一种概念,即寿命早期的 IGF-1 水平为随后的健康寿命和导致衰老的病理变化创造了必要的条件。然而,这些变化是特定于每个性别和组织的。重要的是,老年 IGF-1 缺乏(与人类研究相关的时间点)降低了癌症风险,但不会延长寿命。总的来说,我们的结果表明,发育过程中的 IGF-1 水平影响老年期的病理,表明 IGF-1 是健康寿命、病理和寿命的发育驱动因素。

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