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首页> 外文期刊>Neurobiology of Aging: Experimental and Clinical Research >Hypothalamic neurogenesis persists in the aging brain and is controlled by energy-sensing IGF-I pathway
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Hypothalamic neurogenesis persists in the aging brain and is controlled by energy-sensing IGF-I pathway

机译:下丘脑神经发生持续在衰老的大脑中,并受能量敏感的IGF-I途径控制

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摘要

Hypothalamic tanycytes are specialized glial cells lining the third ventricle. They are recently identified as adult stem and/or progenitor cells, able to self-renew and give rise to new neurons postnatally. However, the long-term neurogenic potential of tanycytes and the pathways regulating lifelong cell replacement in the adult hypothalamus are largely unexplored. Using inducible nestin-CreER(T2) for conditional mutagenesis, we performed lineage tracing of adult hypothalamic stem and/or progenitor cells (HySC) and demonstrated that new neurons continue to be born throughout adult life. This neurogenesis was targeted to numerous hypothalamic nuclei and produced different types of neurons in the dorsal periventricular regions. Some adult-born neurons integrated the median eminence and arcuate nucleus during aging and produced growth hormone releasing hormone. We showed that adult hypothalamic neurogenesis was tightly controlled by insulin-like growth factors (IGF). Knockout of IGF-1 receptor from hypothalamic stem and/or progenitor cells increased neuronal production and enhanced alpha-tanycyte self-renewal, preserving this stem cell-like population from age-related attrition. Our data indicate that adult hypothalamus retains the capacity of cell renewal, and thus, a substantial degree of structural plasticity throughout lifespan. (C) 2016 Elsevier Inc. All rights reserved.
机译:下丘脑单核细胞是位于第三脑室的专门神经胶质细胞。它们最近被鉴定为成年干细胞和/或祖细胞,能够自我更新并在出生后产生新的神经元。但是,在成人下丘脑中,单核细胞的长期神经源性潜力和调节终身细胞置换的途径尚待开发。使用诱导型nestin-CreER(T2)进行条件诱变,我们进行了成年下丘脑干细胞和/或祖细胞(HySC)的谱系追踪,并证明了新的神经元在整个成年后继续出生。这种神经发生作用针对大量下丘脑核,并在背侧脑室周围区域产生不同类型的神经元。一些成年出生的神经元在衰老过程中整合了中位突出和弓形核,并产生了生长激素释放激素。我们表明,成人下丘脑神经发生受到胰岛素样生长因子(IGF)的严格控制。从下丘脑干细胞和/或祖细胞中剔除IGF-1受体可以增加神经元的产生并增强α-单核细胞的自我更新,从而使这种干细胞样的种群免受年龄相关的消耗。我们的数据表明,成人下丘脑保留了细胞更新的能力,因此在整个生命周期中具有相当程度的结构可塑性。 (C)2016 Elsevier Inc.保留所有权利。

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