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Gene expression in the liver of female but not male mice treated with rapamycin resembles changes observed under dietary restriction

机译:用雷帕霉素治疗的雌性小鼠而非雄性小鼠肝脏中的基因表达类似于在饮食限制下观察到的变化

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摘要

It is well known that in mice the extension in lifespan by rapamycin is sexually dimorphic, in that it has a larger effect in females than males. In a previous study we showed that in male C57BL6 mice, rapamycin had less profound effects in both gene expression and liver metabolites when compared to dietary restriction (DR), but no data was available in females. Because recent studies showed that rapamycin increases longevity in a dose dependent manner and at every dose tested the effect remains larger in females than in males, we hypothesized that rapamycin should have a stronger effect on gene expression in females, and this effect could be dose dependent. To test this hypothesis, we measured the changes in liver gene expression induced by rapamycin (14 ppm) with a focus on several genes involved in pathways known to play a role in aging and that are altered by DR. To investigate whether any effects are dose dependent, we also analyzed females treated with two additional doses of rapamycin (22 and 42 ppm). We observed striking differences between male and female in gene expression at 14 ppm, where females have a larger response to rapamycin than males, and the effects of rapamycin in females resemble what we observed under DR. However, these effects were generally not dose dependent. These data support the notion that female mice respond better to rapamycin, and at least with the set of genes studied here, the effect of rapamycin in females resemble the effect of DR.Electronic supplementary materialThe online version of this article (doi:10.1186/s40064-015-0909-7) contains supplementary material, which is available to authorized users.
机译:众所周知,雷帕霉素在小鼠中的寿命延长是有性的,因为它对雌性的作用大于对雄性的作用。在先前的研究中,我们表明,与饮食限制(DR)相比,雷帕霉素在雄性C57BL6小鼠中对基因表达和肝脏代谢产物的影响均较小,但没有雌性的数据。因为最近的研究表明雷帕霉素以剂量依赖性方式增加寿命,并且在每次测试剂量下,雌性药物的作用仍大于雄性,因此我们假设雷帕霉素对雌性基因的表达应具有更强的作用,并且这种作用可能是剂量依赖性的。为了检验这一假设,我们测量了雷帕霉素(14 ppm)诱导的肝基因表达的变化,重点是与已知在衰老中起作用并且被DR改变的通路中涉及的几个基因有关。为了研究是否有任何效应是剂量依赖性的,我们还分析了接受两次额外剂量雷帕霉素(22和42 ppm)治疗的女性。我们观察到男性和女性在14 ppm的基因表达上存在显着差异,其中女性对雷帕霉素的反应比男性要大,雷帕霉素对女性的作用与我们在DR下观察到的相似。但是,这些作用通常与剂量无关。这些数据支持以下观点:雌性小鼠对雷帕霉素的反应更好,并且至少通过此处研究的一组基因,雷帕霉素对雌性小鼠的作用类似于DR的作用。电子补充材料本文的在线版本(doi:10.1186 / s40064 -015-0909-7)包含补充材料,授权用户可以使用。

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