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Sexual differentiation, pregnancy, calorie restriction, and aging affect the adipocyte-specific secretory protein adiponectin.

机译:性别分化,怀孕,卡路里限制和衰老会影响脂肪细胞特异性分泌蛋白脂联素。

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摘要

Adiponectin or adipocyte complement-related protein of 30 kDa (Acrp30) is a circulating protein produced exclusively in adipocytes. Circulating Acrp30 levels have been associated with insulin sensitivity in adult mice and humans, yet the Acrp30 profile over the lifespan and its hormonal regulation in vivo have not been previously described. Hence, we set forth to determine whether hormonal and metabolic changes associated with sexual maturation, reproduction, aging, and calorie restriction affect Acrp30. In mice, Acrp30 levels increase during sexual maturation by 4-fold in males and 10-fold in females. Neonatal castration (CX) allows Acrp30 of adults to reach female levels. CX in adults does not lead to female Acrp30 levels unless glucocorticoid exposure is elevated simultaneously by implant. Ovariectomy of infant mice does not interfere with the pubertal rise of Acrp30. However, ovariectomy in adults increases Acrp30. Estrogen suppressed Acrp30 in mice and 3T3-L1 adipocytes. In parallel to changes in estrogen action, Acrp30 decreased in late gestation but increased in both calorie-restricted and old (anovulatory) mice. The reduction of Acrp30 in lactating dams is consistent with a suppressive effect of prolactin and a stimulating effect of bromocriptine. In summary, Acrp30 levels in serum are under complex hormonal control and may play a key role in determining systemic insulin sensitivity under the respective conditions.
机译:脂联素或30 kDa的脂肪细胞补体相关蛋白(Acrp30)是仅在脂肪细胞中产生的循环蛋白。循环的Acrp30水平已与成年小鼠和人类的胰岛素敏感性相关联,但先前并未描述整个生命中的Acrp30概况及其体内激素调节。因此,我们着手确定与性成熟,生殖,衰老和卡路里限制相关的激素和代谢变化是否会影响Acrp30。在小鼠中,性成熟过程中Acrp30的水平增加,雄性增加4倍,雌性增加10倍。新生儿去势(CX)使成年人的Acrp30达到女性水平。成年人的CX不会导致女性Acrp30水平升高,除非通过植入同时提高糖皮质激素的暴露水平。婴儿小鼠的卵巢切除术不会干扰Acrp30的青春期上升。但是,成人卵巢切除术会增加Acrp30。雌激素抑制小鼠和3T3-L1脂肪细胞中的Acrp30。与雌激素作用的变化同时,Acrp30在妊娠后期降低,但在卡路里受限和年老(无排卵)小鼠中均升高。泌乳坝中Acrp30的减少与催乳素的抑制作用和溴隐亭的刺激作用一致。总之,血清中的Acrp30水平处于复杂的激素控制之下,并可能在确定各种条件下的全身胰岛素敏感性中起关键作用。

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