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衰老相关的中枢调控对短命非洲食蚊鱼 Orexin 和 NPY 的影响。

Age-related central regulation of orexin and NPY in the short-lived African killifish Nothobranchius furzeri.

机构信息

Department of Veterinary Medicine and Animal Productions, University of Naples Federico II, Naples, Italy.

Leibniz-Institute on Aging - Fritz Lipmann Institute (FLI), Lab. Biology of Aging, Jena, Germany.

出版信息

J Comp Neurol. 2019 May 15;527(9):1508-1526. doi: 10.1002/cne.24638. Epub 2019 Feb 13.

Abstract

Orexin A (OXA) and neuropeptide Y (NPY) are two hypothalamic neuropeptides involved in the regulation of feeding behavior and food intake in all vertebrates. Accumulating evidences document that they undergo age-related modifications, with consequences on metabolism, sleep/wake disorders and progression of neurodegenerations. The present study addressed the age related changes in expression and distribution of orexin A (its precursor is also known as hypocretin-HCRT) and NPY, and their regulation by food intake in the short-lived vertebrate model Nothobranchius furzeri. Our experiments, conducted on male specimens, show that: (a) HCRT and OXA and NPY mRNA and protein are localized in neurons of diencephalon and optic tectum, as well as in numerous fibers projecting through the entire neuroaxis, and are colocalized in specific nuclei; (b) in course of aging, HCRT and NPY expressing neurons are localized also in telencephalon and rhombencephalon; (c) HCRT expressing neurons increased slightly in the diencephalic area of old animals and in fasted animals, whereas NPY increased sharply; (d) central HCRT levels are not regulated neither in course of aging nor by food intake; and (e) central NPY levels are augmented in course of aging, and regulated by food intake only in young. These findings represent a great novelty in the study of central orexinergic and NPY-ergic systems in vertebrates', demonstrating an uncommon and unprecedented described regulation of these two orexigenic neuropeptides.

摘要

食欲素 A(OXA)和神经肽 Y(NPY)是两种参与调节所有脊椎动物摄食行为和食物摄入的下丘脑神经肽。越来越多的证据表明,它们会发生与年龄相关的变化,从而对代谢、睡眠/觉醒障碍和神经退行性变的进展产生影响。本研究探讨了寿命较短的脊椎动物模型非洲爪蟾中食欲素 A(其前体也称为下丘脑泌素-HCRT)和 NPY 的表达和分布的年龄相关性变化,以及它们与食物摄入的关系。我们的实验是在雄性标本上进行的,结果表明:(a)HCRT 和 OXA 和 NPY 的 mRNA 和蛋白定位于间脑和视顶盖的神经元中,以及投射穿过整个神经轴的众多纤维中,并且在特定核中共定位;(b)随着年龄的增长,HCRT 和 NPY 表达神经元也定位于端脑和后脑;(c)在老年动物和禁食动物中,HCRT 表达神经元在间脑区域略有增加,而 NPY 则急剧增加;(d)中央 HCRT 水平在衰老过程中不受调节,也不受食物摄入的调节;(e)中央 NPY 水平随着衰老而增加,并且仅在年轻动物中受食物摄入调节。这些发现代表了在研究脊椎动物中枢食欲素能和 NPY 能系统方面的重大新发现,证明了这两种食欲肽神经肽的不常见和前所未有的调节。

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