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首页> 外文期刊>Psychoneuroendocrinology: An International Journal >Ghrelin and hypothalamic NPY/AgRP expression in mice are affected by chronic early-life stress exposure in a sex-specific manner
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Ghrelin and hypothalamic NPY/AgRP expression in mice are affected by chronic early-life stress exposure in a sex-specific manner

机译:小鼠中的Ghrelin和下丘脑NPY / AGRP表达受到性别特异性的慢性早期压力暴露的影响

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摘要

Highlights ? Ghrelin levels are more prominently affected by chronic early-life stress in neonatal female mice compared to males. ? Early-life stress induced alterations in total ghrelin are largely attributed by the desacyl form of ghrelin. ? Hypothalamic NPY/AgRP expression are similarly increased after early-life stress in two-week-old male and female mice. Abstract Early-life stress (ES) is a risk factor for metabolic disorders (e.g. obesity) with a notoriously higher prevalence in women compared to men. However, mechanisms underlying these effects remain elusive. The development of the hypothalamic feeding and metabolic regulatory circuits occurs mostly in the early sensitive postnatal phase in rodents and is tightly regulated by the metabolic hormones leptin and ghrelin. We have previously demonstrated that chronic ES reduces circulating leptin and alters adipose tissue metabolism early and later in life similarly in both sexes. However, it is unknown whether chronic ES might also affect developmental ghrelin and insulin levels, and if it induces changes in hypothalamic feeding circuits, possibly in a sex-dependent manner. We here show that chronic ES, in the form of exposure to limited nesting and bedding material from postnatal day (P)2 to P9 in mice, affects ghrelin levels differently, depending on the form of ghrelin (acylated vs desacylated), on age (P9 vs P14) and on sex, while insulin levels were similarly increased in both sexes after ES at P9. Even though ghrelin levels were more strongly affected in ES-exposed females, hypothalamic neuropeptide Y (NPY) and agouti-related peptide (AgRP) fiber density at P14 were similarly altered in both sexes by ES. In the paraventricular nucleus of the hypothalamus, both NPY and AgRP fiber density were increased, while in the arcuate nucleus of the hypothalamus, NPY was increased and AgRP unaltered. Additionally, the hypothalamic mRNA expression of ghrelin’s receptor (i.e. growth hormone secretagogue receptor) was not affected by ES. Taken together, the specific alterations found in these important regulatory circuits after ES might contribute to an altered energy balance and feeding behavior in adulthood and thereby to an increased vulnerability to develop metabolic disorders.
机译:强调 ?与雄性相比,患有新生儿女性小鼠的慢性早期胁迫的慢性早期胁迫的疟原蛋白水平令人震惊。还预生命应激诱导的总Ghrelin的改变在很大程度上归因于Ghrelin的脱酰基。还在两周老雄性和女性小鼠的早期压力后,下丘脑NPY / AGRP表达类似地增加。摘要早期压力(ES)是代谢障碍(例如肥胖)的危险因素,与男性相比,女性的普令生普遍较高。然而,这些效果的机制仍然难以捉摸。下丘脑喂养和代谢调节电路的发展主要发生在啮齿动物的早期敏感的后期相中,并且由代谢激素瘦素和Ghrelin紧密调节。我们之前已经证明,慢性ES减少了循环瘦素,并在两性中的生活中早期和后期改变了脂肪组织代谢。然而,尚不清楚慢性es也可能影响发育疟疾和胰岛素水平,以及诱导丘脑喂料电路的变化,可能是以性依赖的方式。我们在这里表明,慢性ES,以暴露于小鼠的后期(P)2至P9的暴露于有限的嵌套和床上用品材料,根据Ghrelin(酰化Vs Desacylated)的形式,根据年龄( P9 VS P14)和性别,而在P9的ES后两性在两性中同样增加了胰岛素水平。尽管在ES暴露的女性中,诸如ES暴露的女性的疟原蛋白水平更强烈地影响P14的下丘脑神经肽Y(NPY)和agouti相关的肽(AGRP)纤维密度。在下丘脑的椎间盘核中,NPY和AGRP纤维密度均增加,而在下丘脑的弧形核中,NPY增加并禁止AGRP。另外,Ghrelin受体的下丘脑mRNA表达(即生长激素促分泌素受体)不受ES的影响。在一起,在ES后,在这些重要的监管电路中发现的具体改变可能导致成年期的能量平衡和饲养行为有助于增加脆弱性来开发代谢障碍。

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