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Aging, depot origin, and preadipocyte gene expression.

机译:衰老,长效来源和前脂肪细胞基因表达。

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摘要

Fat distribution changes with aging. Inherent changes in fat cell progenitors may contribute because fat cells turn over throughout life. To define mechanisms, gene expression was profiled in preadipocytes cultured from epididymal and perirenal depots of young and old rats. 8.4% of probe sets differed significantly between depots, particularly developmental genes. Only 0.02% differed with aging, despite using less stringent criteria than for comparing depots. Twenty-five genes selected based on fold change with aging were analyzed in preadipocytes from additional young, middle-aged, and old animals by polymerase chain reaction. Thirteen changed significantly with aging, 13 among depots, and 9 with both. Genes involved in inflammation, stress, and differentiation changed with aging, as occurs in fat tissue. Age-related changes were greater in perirenal than epididymal preadipocytes, consistent with larger declines in replication and adipogenesis in perirenal preadipocytes. Thus, age-related changes in preadipocyte gene expression differ among depots, potentially contributing to fat redistribution and dysfunction.
机译:脂肪分布随年龄而变化。脂肪细胞祖先的固有变化可能是由于脂肪细胞在整个生命过程中都在运转而引起的。为了定义机制,在幼鼠和老鼠的附睾和肾周贮藏物中培养的前脂肪细胞中分析了基因表达。仓库之间,尤其是发育基因之间,有8.4%的探针组存在显着差异。尽管使用的严格标准不如比较仓库,但老化的差异仅为0.02%。通过聚合酶链反应,从另外的年幼,中年和老年动物的前脂肪细胞中分析了基于衰老倍数选择的25个基因。十三随着老化而显着变化,仓库之间的变化为十三,两者之间的变化为九。炎症,压力和分化相关的基因会随着年龄的增长而发生变化,就像在脂肪组织中一样。与附睾前脂肪细胞相比,肾周的年龄相关变化更大,这与肾周脂肪细胞中复制和脂肪生成的下降较大有关。因此,不同年龄段的前脂肪细胞基因表达的年龄相关变化是不同的,可能导致脂肪重新分布和功能障碍。

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