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长寿的αMUPA小鼠在寿命、能量及昼夜节律稳态相关参数方面表现出性二态性降低。

Long-Lived αMUPA Mice Show Reduced Sexual Dimorphism in Lifespan, and in Energy and Circadian Homeostasis-Related Parameters.

作者信息

Steckler Rafi, Shabtay-Yanai Ateret, Pinsky Mariel, Rauch Maayan, Tamir Snait, Gutman Roee

机构信息

Unit of Integrative Physiology (LIP), Laboratory of Human Health and Nutrition Sciences, MIGAL - Galilee Research Institute, Kiryat Shmona, Israel. Department of Nutritional Sciences, Tel-Hai College, Upper Galilee, Israel.

Unit of Integrative Physiology (LIP), Laboratory of Human Health and Nutrition Sciences, MIGAL - Galilee Research Institute, Kiryat Shmona, Israel.

出版信息

J Gerontol A Biol Sci Med Sci. 2016 Apr;71(4):451-60. doi: 10.1093/gerona/glv019. Epub 2015 Apr 11.

Abstract

Female αMUPA (alpha murine urokinase-like plasminogen activator) transgenic mice show increased lifespan, reduced body weight and food intake, and high-amplitude circadian rhythms with an endogenous period length (tau) of 24h, versus their wild types (WT) showing a 23.7-h tau. Our goal was to characterize αMUPA and WT male mice, and their in-strain sexual dimorphism, and to further understand the mechanisms underlying αMUPA's longevity. Male αMUPA mice showed increased lifespan, reduced body weight and food intake, and aligned endogenous rhythm with a tau of 24.0h versus a tau <24h in WT. However, no differences were found when intake was corrected for metabolic mass in male αMUPA mice. αMUPA's sexual dimorphism was damped or lacking in all studied traits, while WTs were sexually dimorphic, concluding that αMUPA's transgene overrides sex-dependent mechanisms involved in lifespan and in energy and circadian homeostasis. As enhanced resonance between tau and external circadian cycle correlates with increased lifespan and reduced body weight in other species, including humans, αMUPA's 24-h tau could contribute to their longevity. Focusing future research on the mechanistic interconnections between energy homeostasis, circadian homeostasis, sexual dimorphism, and aging, using αMUPA mice, may reveal mechanisms promoting reduced body weight and increased lifespan.

摘要

与野生型(WT)小鼠相比,雌性αMUPA(α-小鼠尿激酶样纤溶酶原激活剂)转基因小鼠寿命延长、体重和食物摄入量降低,且具有24小时的内源性周期长度(tau)的高振幅昼夜节律,而野生型小鼠的tau为23.7小时。我们的目标是对αMUPA和野生型雄性小鼠及其品系内的性别二态性进行表征,并进一步了解αMUPA长寿的潜在机制。雄性αMUPA小鼠寿命延长、体重和食物摄入量降低,内源性节律与24.0小时的tau对齐,而野生型小鼠的tau<24小时。然而,在对雄性αMUPA小鼠的代谢质量进行校正后,未发现摄入量有差异。在所有研究的性状中,αMUPA的性别二态性减弱或不存在,而野生型小鼠具有性别二态性,得出的结论是,αMUPA的转基因超越了与寿命、能量和昼夜节律稳态相关的性别依赖机制。由于在包括人类在内的其他物种中,tau与外部昼夜周期之间增强的共振与寿命延长和体重减轻相关,αMUPA的24小时tau可能有助于其长寿。利用αMUPA小鼠,将未来的研究重点放在能量稳态、昼夜节律稳态、性别二态性和衰老之间的机制联系上,可能会揭示促进体重减轻和寿命延长的机制。

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