Cheng Hua, Mancuso David J, Jiang Xuntian, Guan Shaoping, Yang Jingyue, Yang Kui, Sun Gang, Gross Richard W, Han Xianlin
Division of Bioorganic Chemistry and Molecular Pharmacology, Department of Internal Medicine, Washington University School of Medicine, St. Louis, Missouri 63110, USA.
Biochemistry. 2008 May 27;47(21):5869-80. doi: 10.1021/bi7023282. Epub 2008 May 3.
Large-scale neuronal remodeling through apoptosis occurs shortly after birth in all known mammalian species. Apoptosis, in large part, depends upon critical interactions between mitochondrial membranes and cytochrome c. Herein, we examined the hypothesis that the large-scale reorganization of neuronal circuitry after birth is accompanied by profound alterations in cardiolipin (CL) content and molecular species distribution. During embryonic development, over 100 CL molecular species were identified and quantitated in murine neuronal tissues. The embryonic CL profile was notable for the presence of abundant amounts of relatively short aliphatic chains (e.g., palmitoleic and oleic acids). In sharp contrast, after birth, the CL profile contained a remarkably complex repertoire of CL molecular species, in which the signaling fatty acids (i.e., arachidonic and docosahexaenoic acids) were markedly increased. These results identify the rapid remodeling of CL in the perinatal period with resultant alterations in the physical properties of the mitochondrial membrane. The complex distribution of aliphatic chains in the neuronal CL pool is separate and distinct from that in other organs (e.g., heart, liver, etc.), where CL molecular species contain predominantly only one major type of aliphatic chain (e.g., linoleic acid). Analyses of mRNA levels by real-time quantitative polymerase chain reactions suggested that the alterations in CL content were due to the combined effects of both attenuation of de novo CL biosynthesis and decreased remodeling of CL. Collectively, these results provide a new perspective on the complexity of CL in neuronal signaling, mitochondrial bioenergetics, and apoptosis.
在所有已知的哺乳动物物种中,出生后不久就会通过细胞凋亡发生大规模的神经元重塑。细胞凋亡在很大程度上取决于线粒体膜与细胞色素c之间的关键相互作用。在此,我们检验了这样一种假说,即出生后神经元回路的大规模重组伴随着心磷脂(CL)含量和分子种类分布的深刻改变。在胚胎发育过程中,在小鼠神经元组织中鉴定并定量了100多种CL分子种类。胚胎期的CL谱以存在大量相对短的脂肪链(如棕榈油酸和油酸)为特征。与之形成鲜明对比的是,出生后,CL谱包含了一个非常复杂的CL分子种类库,其中信号脂肪酸(即花生四烯酸和二十二碳六烯酸)显著增加。这些结果表明围产期CL的快速重塑导致线粒体膜物理性质的改变。神经元CL库中脂肪链的复杂分布与其他器官(如心脏、肝脏等)中的分布是分开且不同的,在其他器官中,CL分子种类主要只包含一种主要类型的脂肪链(如亚油酸)。通过实时定量聚合酶链反应对mRNA水平的分析表明,CL含量的改变是由于从头合成CL的减弱和CL重塑减少的综合作用。总的来说,这些结果为CL在神经元信号传导、线粒体生物能量学和细胞凋亡中的复杂性提供了一个新的视角。