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Hypothalamic gene transfer of BDNF promotes healthy aging in mice

机译:BDNF的下丘脑基因转移促进小鼠健康衰老

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摘要

The aging process and age‐related diseases all involve perturbed energy adaption and impaired ability to cope with adversity. Brain‐derived neurotrophic factor (BDNF) in the hypothalamus plays important role in regulation of energy balance. Our previous studies show that recombinant adeno‐associated virus (AAV)‐mediated hypothalamic BDNF gene transfer alleviates obesity, diabetes, and metabolic syndromes in both diet‐induced and genetic models. Here we examined the efficacy and safety of a built‐in autoregulatory system to control transgene BDNF expression mimicking the body's natural feedback systems in middle‐aged mice. Twelve‐month‐old mice were treated with either autoregulatory BDNF vector or yellow fluorescence protein (YFP) control, maintained on normal diet, and monitored for 28 weeks. BDNF gene transfer prevented the development of aging‐associated metabolic declines characterized by: preventing aging‐associated weight gain, reducing adiposity, reversing the decline of brown fat activity, increasing adiponectin while reducing leptin and insulin in circulation, improving glucose tolerance, increasing energy expenditure, alleviating hepatic steatosis, and suppressing inflammatory genes in the hypothalamus and adipose tissues. Moreover, BDNF treatment reduced anxiety‐like and depression‐like behaviors. These safety and efficacy data provide evidence that hypothalamic BDNF is a target for promoting healthy aging.
机译:衰老过程和与年龄有关的疾病都涉及能量适应和应对逆境的能力受损。下丘脑的脑源性神经营养因子(BDNF)在调节能量平衡中起重要作用。我们以前的研究表明,在饮食诱导和遗传模型中,重组腺相关病毒(AAV)介导的下丘脑BDNF基因转移均可减轻肥胖,糖尿病和代谢综合征。在这里,我们研究了内置自动调节系统控制转基因BDNF表达的功效和安全性,该表达模仿了中年小鼠体内的自然反馈系统。用自动调节的BDNF载体或黄色荧光蛋白(YFP)对照治疗12个月大的小鼠,维持正常饮食,并监测28周。 BDNF基因转移阻止了与衰老相关的代谢下降,其特征是:防止与衰老相关的体重增加,减少肥胖,逆转棕色脂肪活性的下降,增加脂联素同时减少循环中的瘦素和胰岛素,改善葡萄糖耐量,增加能量消耗,减轻肝脏脂肪变性,并抑制下丘脑和脂肪组织中的炎症基因。此外,BDNF治疗可减少焦虑症和抑郁症的行为。这些安全性和有效性数据提供了下丘脑BDNF是促进健康衰老的目标的证据。

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