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神经元培养微环境决定生物能量途径使用偏好。

Neuronal Culture Microenvironments Determine Preferences in Bioenergetic Pathway Use.

作者信息

Sünwoldt Juliane, Bosche Bert, Meisel Andreas, Mergenthaler Philipp

机构信息

Charité - Universitätsmedizin Berlin, Department of Experimental Neurology, Berlin, Germany.

Division of Neurosurgery, Keenan Research Centre for Biomedical Science and the Li Ka Shing Knowledge Institute, St. Michael's Hospital, University of Toronto, Toronto, ON, Canada.

出版信息

Front Mol Neurosci. 2017 Sep 29;10:305. doi: 10.3389/fnmol.2017.00305. eCollection 2017.

Abstract

In the brain, metabolic supply and demand is directly coupled to neuronal activation. Methods for culturing primary rodent brain cells have come of age and are geared toward sophisticated modeling of human brain physiology and pathology. However, the impact of the culture microenvironment on neuronal function is rarely considered. Therefore, we investigated the role of different neuronal culture supplements for neuronal survival and metabolic activity in a model of metabolic deprivation of neurons using oxygen deprivation, glucose deprivation, as well as live cell metabolic flux analysis. We demonstrate the impact of neuronal culture conditions on metabolic function and neuronal survival under conditions of metabolic stress. In particular, we find that the common neuronal cell culture supplement B27 protects neurons from cell death under hypoxic conditions and inhibits glycolysis. Furthermore, we present data that B27 as well as the alternative neuronal culture supplement N2 restrict neuronal glucose metabolism. On the contrary, we find that the more modern supplement GS21 promotes neuronal energy metabolism. Our data support the notion that careful control of the metabolic environment is an essential component in modeling brain function and the cellular and molecular pathophysiology of brain disease in culture.

摘要

在大脑中,代谢供应与需求直接与神经元激活相关联。原代啮齿动物脑细胞的培养方法已经成熟,旨在对人类大脑生理和病理进行复杂建模。然而,培养微环境对神经元功能的影响却很少被考虑。因此,我们使用缺氧、葡萄糖剥夺以及活细胞代谢通量分析,在神经元代谢剥夺模型中研究了不同神经元培养补充剂对神经元存活和代谢活性的作用。我们证明了在代谢应激条件下神经元培养条件对代谢功能和神经元存活的影响。特别是,我们发现常见的神经元细胞培养补充剂B27在缺氧条件下可保护神经元免于细胞死亡并抑制糖酵解。此外,我们提供的数据表明B27以及替代神经元培养补充剂N2会限制神经元葡萄糖代谢。相反,我们发现更现代的补充剂GS21可促进神经元能量代谢。我们的数据支持这样一种观点,即在培养中对代谢环境进行仔细控制是模拟脑功能以及脑部疾病的细胞和分子病理生理学的重要组成部分。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/6370/5649214/05d2b27bc63c/fnmol-10-00305-g001.jpg

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