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热量限制:从汤到坚果。

Caloric restriction: from soup to nuts.

机构信息

Department of Biochemistry, University of California, Riverside, Riverside, CA, USA.

出版信息

Ageing Res Rev. 2010 Jul;9(3):324-53. doi: 10.1016/j.arr.2009.10.003. Epub 2009 Oct 21.

DOI:10.1016/j.arr.2009.10.003
PMID:19853062
Abstract

Caloric restriction (CR), reduced protein, methionine, or tryptophan diets; and reduced insulin and/or IGFI intracellular signaling can extend mean and/or maximum lifespan and delay deleterious age-related physiological changes in animals. Mice and flies can shift readily between the control and CR physiological states, even at older ages. Many health benefits are induced by even brief periods of CR in flies, rodents, monkeys, and humans. In humans and nonhuman primates, CR produces most of the physiologic, hematologic, hormonal, and biochemical changes it produces in other animals. In primates, CR provides protection from type 2 diabetes, cardiovascular and cerebral vascular diseases, immunological decline, malignancy, hepatotoxicity, liver fibrosis and failure, sarcopenia, inflammation, and DNA damage. It also enhances muscle mitochondrial biogenesis, affords neuroprotection; and extends mean and maximum lifespan. CR rapidly induces antineoplastic effects in mice. Most claims of lifespan extension in rodents by drugs or nutrients are confounded by CR effects. Transcription factors and co-activators involved in the regulation of mitochondrial biogenesis and energy metabolism, including SirT1, PGC-1alpha, AMPK and TOR may be involved in the lifespan effects of CR. Paradoxically, low body weight in middle aged and elderly humans is associated with increased mortality. Thus, enhancement of human longevity may require pharmaceutical interventions.

摘要

热量限制(CR)、减少蛋白质、蛋氨酸或色氨酸饮食;以及减少胰岛素和/或 IGFI 细胞内信号传导,可以延长动物的平均寿命和最大寿命,并延缓与年龄相关的有害生理变化。即使在老年时,老鼠和苍蝇也可以很容易地在对照和 CR 生理状态之间转换。即使是短暂的 CR 也能在苍蝇、啮齿动物、猴子和人类中诱导许多健康益处。在人类和非人类灵长类动物中,CR 产生的生理、血液、激素和生化变化与其他动物相似。在灵长类动物中,CR 可预防 2 型糖尿病、心血管和脑血管疾病、免疫衰退、恶性肿瘤、肝毒性、肝纤维化和衰竭、肌肉减少症、炎症和 DNA 损伤。它还增强了肌肉线粒体生物发生,提供神经保护,并延长平均和最大寿命。CR 可迅速在小鼠中诱导抗肿瘤作用。大多数药物或营养物质延长啮齿动物寿命的说法都受到 CR 效应的混淆。参与线粒体生物发生和能量代谢调节的转录因子和共激活因子,包括 SirT1、PGC-1alpha、AMPK 和 TOR,可能参与 CR 对寿命的影响。矛盾的是,中年和老年人的低体重与死亡率增加有关。因此,增强人类的长寿可能需要药物干预。

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