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首页> 外文期刊>Biogerontology >Ovariectomy causes immunosenescence and oxi-inflamm-ageing in peritoneal leukocytes of aged female mice similar to that in aged males
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Ovariectomy causes immunosenescence and oxi-inflamm-ageing in peritoneal leukocytes of aged female mice similar to that in aged males

机译:卵巢切除术导致老年雌性小鼠腹膜白细胞的免疫衰老和氧化性炎症类似于老年雄性小鼠

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摘要

Immunosenescence involves age-associated restructuring changes of innate and adaptative immune functions. We have suggested that these changes of the immune system participate in the rate of ageing through modulating oxi-inflamm-ageing. Thus, age-related changes in the immune system can be biological age markers and predictors of longevity. Gender differences in oxidation status and immune functions have been observed in rats, with males showing higher oxidation and immunosenescence than females of the same age. Oestrogens are sex hormones that actively participate in modulating the mammalian immune function and, therefore, the age-related impairment of the immune response is drastically accelerated in females during the menopausal transition. Ovariectomy in rodents constitutes a good model for mimicking human oestrogen loss and thus the menopausal situation. Recently, we have shown the deleterious effects of oestrogen loss on several functions of leukocytes from immune organs in rats and mice. In addition, ovariectomised rats show similar levels in these immune functions to those in males. The present work studied several functions as well as inflammatory and oxidative stress parameters in mouse peritoneal macrophages and lymphocytes from old sham and ovariectomised females, as well as in males of the same age. In general, the results show that females, which have a higher immune response and a lower oxidation and inflammation than males, appear similar to males in the parameters studied when they have lost oestrogens by ovariectomy. Thus, these data support the positive role of oestrogens in the immune function through the ageing process.
机译:免疫衰老涉及与年龄相关的先天和适应性免疫功能的重组变化。我们已经提出,免疫系统的这些变化通过调节氧化性-炎症-老化来参与衰老的速率。因此,免疫系统中与年龄相关的变化可能是生物学的年龄标记和寿命的预测因子。在大鼠中观察到了氧化状态和免疫功能的性别差异,其中雄性显示出比同龄雌性更高的氧化和免疫衰老。雌激素是积极参与调节哺乳动物免疫功能的性激素,因此,在绝经期过渡期,雌性动物的年龄相关免疫反应损害显着加速。在啮齿动物中进行卵巢切除术是模仿人类雌激素流失和更年期情况的良好模型。最近,我们已经显示雌激素损失对大鼠和小鼠免疫器官中白细胞的几种功能的有害作用。此外,去卵巢大鼠在这些免疫功能中的水平与男性相似。目前的工作研究了小鼠假性和卵巢切除的雌性小鼠以及同龄雄性小鼠的腹膜巨噬细胞和淋巴细胞中的几种功能以及炎性和氧化应激参数。总的来说,结果表明,在卵巢切除术中失去雌激素的女性中,与男性相比,具有更高的免疫应答,更低的氧化和炎症反应的女性看起来与男性相似。因此,这些数据支持了雌激素在衰老过程中在免疫功能中的积极作用。

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