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首页> 外文期刊>Brain research >Hypothalamic kiss1 mRNA and kisspeptin immunoreactivity are reduced in a rat model of polycystic ovary syndrome (PCOS)
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Hypothalamic kiss1 mRNA and kisspeptin immunoreactivity are reduced in a rat model of polycystic ovary syndrome (PCOS)

机译:下丘脑kiss1 mRNA和kisepteptin免疫反应性在多囊卵巢综合征(PCOS)大鼠模型中降低

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An intact hypothalamic kiss1/kisspeptin/kiss1r complex is a prerequisite for reproductive competence, and kisspeptin treatment could be a practical therapeutic approach to some problems of infertility. One such disorder is polycystic ovarian syndrome (PCOS), a common cause of infertility affecting more than 100 million women. A rodent model of PCOS is the prepubertal female rat treated for a prolonged period with dihydrotestosterone (DHT), which induces many of the metabolic characteristics of the syndrome. We hypothesized that hypothalamic kiss1 mRNA levels, and kisspeptin immunoreactivity (ir), would be abnormal in these rats. Prepubertal female rats were exposed to DHT for 60 days. Rats were killed in two groups: at 26 and 60 days of DHT exposure. Kiss1 mRNA was quantified in hypothalamus, pituitary, ovary and visceral adipose tissue. Separate groups of rats provided brain tissue for immunohistochemical analysis of kisspeptin-ir. At 26 days of DHT exposure, hypothalamic kiss1 mRNA was severely depleted. In contrast DHT had no effect on pituitary kiss1 expression but it significantly increased levels of kiss1 mRNA in fat (+ 9-fold; p < 0.01) and in ovary (+ 3-fold; p < 0.05). At 60 days, kiss1 expression had reverted to normal in hypothalamus and ovary but remained elevated in fat (+ 4-fold; p < 0.05). Immunohistochemical analysis revealed that after 26 days of exposure to DHT, kisspeptin-ir was almost completely absent in the arcuate nucleus and a large depletion in kisspeptin + ve fibers was also seen in the paraventricular nucleus, supraoptic nucleus and in the anteroventral periventricular area. At 60 days, despite restored normal levels of kiss1 mRNA, hypothalamic kisspeptin-ir remained depleted in the treated rats. In summary Kiss1 gene expression is differentially affected in various tissues by chronic exposure to dihydrotestosterone in a rat model of polycystic ovary syndrome. In hypothalamus, specifically, kiss1 mRNA, and levels of kisspeptin immunoreactivity, are significantly reduced. Since these rats exhibit many of the characteristics of polycystic ovary syndrome, we suggest that atypical kiss1 expression may contribute to the multiple tissue abnormalities observed in women with this disorder. However, and of some importance, our data do not appear to be consistent with the elevated levels of LH seen in women with PCOS; i.e. reduced levels of hypothalamic kiss1 mRNA and kisspeptin immunoreactivity observed in DHT-treated rats are unlikely to produce elevated LH secretion.
机译:完整的下丘脑kiss1 / kisspeptin / kiss1r复合体是生殖能力的先决条件,而kisseptin治疗可能是治疗某些不育问题的实用方法。一种这样的疾病是多囊卵巢综合征(PCOS),这是不育症的常见原因,影响了超过1亿妇女。 PCOS的啮齿动物模型是青春期前的雌性大鼠用二氢睾丸激素(DHT)进行了长时间治疗,该诱导了该综合征的许多代谢特征。我们假设这些大鼠的下丘脑kiss1 mRNA水平和kisepteptin免疫反应性(ir)会异常。青春期前的雌性大鼠暴露于DHT 60天。将大鼠分为两组:DHT暴露26天和60天。 Kiss1 mRNA在下丘脑,垂体,卵巢和内脏脂肪组织中定量。分开的大鼠组提供脑组织用于kisspeptin-ir的免疫组织化学分析。在暴露DHT的第26天,下丘脑kiss1 mRNA严重耗尽。相比之下,DHT对垂体kiss1表达没有影响,但会显着增加脂肪中kiss1 mRNA水平(+ 9倍; p <0.01)和卵巢中(+ 3倍; p <0.05)。在60天时,下丘脑和卵巢中kiss1的表达已恢复正常,但脂肪中的亲吻仍保持升高(+ 4倍; p <0.05)。免疫组织化学分析显示,暴露于DHT 26天后,弓形核几乎完全不存在kisseptin-ir,并且在室旁核,视上核和前室周围区域也见到kisepteptin + ve纤维大量消耗。在第60天,尽管kiss1 mRNA恢复正常水平,但下丘脑kisepteptin-ir在治疗大鼠中仍被耗尽。总之,在多囊卵巢综合症的大鼠模型中,慢性暴露于二氢睾丸激素会在各种组织中对Kiss1基因表达产生不同的影响。特别是在下丘脑中,kiss1 mRNA和Kisspeptin免疫反应性水平显着降低。由于这些大鼠表现出多囊卵巢综合征的许多特征,我们建议非典型kiss1表达可能导致患有这种疾病的女性中观察到的多种组织异常。然而,并且在某种程度上,我们的数据似乎与患有PCOS的女性中LH水平升高并不一致。即在DHT处理的大鼠中观察到的下丘脑kiss1 mRNA水平降低和kisspeptin免疫反应性不太可能产生升高的LH分泌。

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