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在灌注过程中,神经元线粒体形态受到固定剂和氧水平的显著影响。

Neuronal mitochondrial morphology is significantly affected by both fixative and oxygen level during perfusion.

作者信息

Kim Su Yeon, Strucinska Klaudia, Osei Bertha, Han Kihoon, Kwon Seok-Kyu, Lewis Tommy L

机构信息

Brain Science Institute, Korea Institute of Science and Technology (KIST), Seoul, South Korea.

Department of Neuroscience, College of Medicine, Korea University, Seoul, South Korea.

出版信息

Front Mol Neurosci. 2022 Nov 2;15:1042616. doi: 10.3389/fnmol.2022.1042616. eCollection 2022.

Abstract

Neurons in the brain have a uniquely polarized structure consisting of multiple dendrites and a single axon generated from a cell body. Interestingly, intracellular mitochondria also show strikingly polarized morphologies along the dendrites and axons: in cortical pyramidal neurons (PNs), dendritic mitochondria have a long and tubular shape, while axonal mitochondria are small and circular. Mitochondria play important roles in each compartment of the neuron by generating adenosine triphosphate (ATP) and buffering calcium, thereby affecting synaptic transmission and neuronal development. In addition, mitochondrial shape, and thereby function, is dynamically altered by environmental stressors such as oxidative stress or in various neurodegenerative diseases including Alzheimer's disease and Parkinson's disease. Although the importance of altered mitochondrial shape has been claimed by multiple studies, methods for studying this stress-sensitive organelle have not been standardized. Here we address pertinent steps that influence mitochondrial morphology during experimental processes. We demonstrate that fixative solutions containing only paraformaldehyde (PFA), or that introduce hypoxic conditions during the procedure, induce dramatic fragmentation of mitochondria both and . This disruption was not observed following the use of glutaraldehyde (GA) addition or oxygen supplementation, respectively. Finally, using pre-formed fibril α-synuclein treated neurons, we show fixative choice can alter experimental outcomes. Specifically, α-synuclein-induced mitochondrial remodeling could not be observed with PFA only fixation as fixation itself caused mitochondrial fragmentation. Our study provides optimized methods for examining mitochondrial morphology in neurons and demonstrates that fixation conditions are critical when investigating the underlying cellular mechanisms involving mitochondria in physiological and neurodegenerative disease models.

摘要

大脑中的神经元具有独特的极化结构,由多个树突和从细胞体发出的单个轴突组成。有趣的是,细胞内的线粒体在树突和轴突上也呈现出明显的极化形态:在皮质锥体神经元(PNs)中,树突线粒体呈长管状,而轴突线粒体则小而呈圆形。线粒体通过产生三磷酸腺苷(ATP)和缓冲钙在神经元的每个部分发挥重要作用,从而影响突触传递和神经元发育。此外,线粒体的形状以及功能会因氧化应激等环境应激因素或包括阿尔茨海默病和帕金森病在内的各种神经退行性疾病而动态改变。尽管多项研究都表明线粒体形态改变的重要性,但研究这种对压力敏感的细胞器的方法尚未标准化。在这里,我们阐述了实验过程中影响线粒体形态的相关步骤。我们证明,仅含有多聚甲醛(PFA)的固定液,或在操作过程中引入缺氧条件,都会导致线粒体在树突和轴突上发生显著碎片化。分别使用添加戊二醛(GA)或补充氧气后未观察到这种破坏。最后,使用预先形成的原纤维α-突触核蛋白处理的神经元,我们表明固定剂的选择会改变实验结果。具体而言,仅用PFA固定时无法观察到α-突触核蛋白诱导的线粒体重塑,因为固定本身会导致线粒体碎片化。我们的研究提供了用于检查神经元中线粒体形态的优化方法,并表明在研究生理和神经退行性疾病模型中涉及线粒体的潜在细胞机制时,固定条件至关重要。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/d7c4/9667081/7d17ce0b01ad/fnmol-15-1042616-g001.jpg

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