首页> 美国卫生研究院文献>Scientific Reports >Kisspeptin/Neurokinin B/Dynorphin (KNDy) cells as integrators of diverse internal and external cues: evidence from viral-based monosynaptic tract-tracing in mice
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Kisspeptin/Neurokinin B/Dynorphin (KNDy) cells as integrators of diverse internal and external cues: evidence from viral-based monosynaptic tract-tracing in mice

机译:Kisspeptin /神经激肽B / Dynorphin(KNDy)细胞作为各种内部和外部线索的整合者:小鼠中基于病毒的单突触道追踪的证据

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摘要

Neurons in the hypothalamic arcuate nucleus (ARC) that co-express kisspeptin, neurokinin B and dynorphin (KNDy cells) are essential for mammalian reproduction as key regulators of gonadotropin-releasing hormone (GnRH) secretion. Although multiple endogenous and exogenous signals act indirectly via KNDy neurons to regulate GnRH, the identity of upstream neurons that provide synaptic input to this subpopulation is unclear. We used rabies-mediated tract-tracing in transgenic Kiss1-Cre mice combined with whole-brain optical clearing and multiple-label immunofluorescence to create a comprehensive and quantitative brain-wide map of neurons providing monosynaptic input to KNDy cells, as well as identify the estrogen receptor content and peptidergic phenotype of afferents. Over 90% of monosynaptic input to KNDy neurons originated from hypothalamic nuclei in both male and female mice. The greatest input arose from non-KNDy ARC neurons, including proopiomelanocortin-expressing cells. Significant female-dominant sex differences in afferent input were detected from estrogen-sensitive hypothalamic nuclei critical for reproductive endocrine function and sexual behavior in mice, indicating KNDy cells may provide a unique site for the coordination of sex-specific behavior and gonadotropin release. These data provide key insight into the structural framework underlying the ability of KNDy neurons to integrate endogenous and environmental signals important for the regulation of reproductive function.
机译:下丘脑弓状核(ARC)中的神经元共同表达Kisspeptin,神经激肽B和强啡肽(KNDy细胞)对于哺乳动物的繁殖至关重要,是促性腺激素释放激素(GnRH)分泌的关键调节剂。尽管多个内源性和外源性信号通过KNDy神经元间接作用来调节GnRH,但尚不清楚为该亚群提供突触输入的上游神经元的身份。我们在转基因的Kiss1-Cre小鼠中使用狂犬病介导的道追踪,并结合了全脑光学清除和多标记免疫荧光技术,以创建全面而定量的全脑神经元图谱,向KNDy细胞提供单突触输入,并鉴定雌激素受体的含量和传入的肽能表型。在雄性和雌性小鼠中,超过90%的KNDy神经元单突触输入均来自下丘脑核。最大的输入来自非KNDy ARC神经元,包括表达proopiomelanocortin的细胞。从雌激素敏感性下丘脑核对小鼠生殖内分泌功能和性行为至关重要,在传入输入中检测到显着的雌性性别差异,表明KNDy细胞可能为协调性别特异性行为和促性腺激素释放提供独特的位点。这些数据为了解KNDy神经元整合对调节生殖功能至关重要的内源性和环境信号能力的结构框架提供了重要见识。

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