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Different Statistical Approaches to Characterization of Adipocyte Size in Offspring of Obese Rats: Effects of Maternal or Offspring Exercise Intervention

机译:肥胖大鼠后代脂肪细胞大小表征的不同统计方法:母体或后代运动干预的影响

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摘要

Adipocyte size (AS) shows asymmetric distribution related to current metabolic state, e.g., adipogenesis or lipolysis. We profiled AS distribution using different statistical approaches in offspring (F1) of control (C) and obese (MO) mothers (F0) with and without F0 or F1 exercise. Offspring from F0 exercise were designated CF0ex and MOF0ex. Exercised F1 of sedentary mothers were designated CF1ex and MOF1ex. F1 retroperitoneal fat cross-sectional AS was measured by median, cumulative distributions, data dispersion and extreme values based on gamma distribution modeling. F1 metabolic parameters: body weight, retroperitoneal fat, adiposity index (AI), serum leptin, triglycerides (TG) and insulin resistance index (IRI) were measured. Male and female F1 AS showed different cumulative distribution between C and MO (p < 0.0001) therefore comparisons were performed among C, CF0ex and CF1ex groups and MO, MOF0ex and MOF1ex groups. MO AI was higher than C (p < 0.05) and male MOF1ex AI lower than MO (p < 0.05). Median AS was higher in male and female MO vs. C (p < 0.05). Male and female MOF0ex and MOF1ex reduced median AS (p < 0.05). Lower AS dispersion was observed in male CF1ex and MOF1ex vs. CF0ex and MOF0ex, respectively. MO reduced small and increased large adipocyte proportions vs. C (p < 0.05); MOF0ex increased small and MOF1ex the proportion of large adipocytes vs. MO (p < 0.05). MOF0ex reduced male IRI and female TG vs. MO (p < 0.05). MOF1ex reduced male and female leptin (p < 0.05); CF1ex reduced male leptin (p < 0.05). Conclusions: several factors, diet, physical activity and gender modify AS distribution. Conventional AS distribution methods normally do not include analyzes of extreme, large and small adipocytes, which characterize different phenotypes. Maternal high fat diet affects F1 AS distribution, which was programmed during development. F0ex and F1ex have gender specific F1 beneficial effects. AS distribution characterization helps explain adipose tissue metabolic changes in different physiological conditions and will aid design of efficacious interventions to prevent and/or recuperate adverse developmental programming outcomes. Finally, precise identification of effects of specific interventions as exercise of F0 and/or F1 are needed to improve outcomes in obese women and their obesity prone offspring.
机译:脂肪细胞大小(AS)显示与当前代谢状态(例如脂肪形成或脂肪分解)相关的不对称分布。我们采用了不同的统计方法,对有或没有进行F0或F1锻炼的对照(C)和肥胖(MO)母亲(F0)的后代(F1)进行了AS分布分析。 F0运动的后代称为CF0ex和MOF0ex。久坐不动的母亲的运动F1称为CF1ex和MOF1ex。 F1腹膜后脂肪横断面AS是根据伽玛分布模型通过中位数,累积分布,数据离散度和极值来测量的。 F1代谢参数:体重,腹膜后脂肪,肥胖指数(AI),血清瘦素,甘油三酸酯(TG)和胰岛素抵抗指数(IRI)。男性和女性F1 AS在C和MO之间显示出不同的累积分布(p <0.0001),因此在C,CF0ex和CF1ex组以及MO,MOF0ex和MOF1ex组之间进行了比较。 MO AI高于C(p <0.05),而男性MOF1ex AI低于MO(p <0.05)。男性和女性MO的AS中位数AS高于C(p <0.05)。男性和女性MOF0ex和MOF1ex降低了中位数AS(p <0.05)。与CF0ex和MOF0ex相比,雄性CF1ex和MOF1ex的AS分散性较低。与C相比,MO降低了小脂肪细胞比例,增加了大脂肪细胞比例(p <0.05);与MO相比,MOF0ex增加了小脂肪细胞的比例,而MOF1ex增加了大脂肪细胞的比例(p <0.05)。与MO相比,MOF0ex降低了男性IRI和女性TG(p <0.05)。 MOF1ex降低了男性和女性的瘦素(p <0.05); CF1ex减少了男性瘦素(p <0.05)。结论:饮食,身体活动和性别等多种因素会改变AS的分布。常规的AS分配方法通常不包括分析表征不同表型的极端,大型和小型脂肪细胞。孕妇高脂饮食会影响F1 AS的分布,这是在发育过程中制定的。 F0ex和F1ex具有针对性别的F1有益效果。 AS分布特征有助于解释脂肪组织在不同生理条件下的代谢变化,并有助于有效干预措施的设计,以预防和/或恢复不良的发育计划结果。最后,需要精确识别运动为F0和/或F1时特定干预措施的效果,以改善肥胖妇女及其肥胖易生后代的结局。

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