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细胞色素 c 与心磷脂在非极性环境中的复合物结构。

Structure of the complex of cytochrome c with cardiolipin in non-polar environment.

机构信息

M.V. Lomonosov Moscow State University, Faculty of Fundamental Medicine, Leninskiye gory 1-3, 119991 Moscow, Russian Federation; Shubnikov Institute of Crystallography of Federal Scientific Research Centre "Crystallography and Photonics" of Russian Academy of Sciences, Leninskiy pr-t 59, 119333 Moscow, Russian Federation; First Moscow State Medical University of the Ministry of Health of the Russian Federation (Sechenov University), Bolshaya Pirogovskaya st. 2-4, 119991 Moscow, Russian Federation.

Nottingham Trent University, School of Science and Technology, Clifton Lane, Nottingham NG11 8NS, UK; Fraunhofer Institute for Cell Therapy and Immunology, Branch Bioanalytics and Bioprocesses (Fraunhofer IZI-BB), Am Muehlenberg 13, 14476 Potsdam-Golm, Germany.

出版信息

Chem Phys Lipids. 2018 Aug;214:35-45. doi: 10.1016/j.chemphyslip.2018.05.007. Epub 2018 May 29.

Abstract

The complex of mitochondrial protein cytochrome c (CytC) with anionic phospholipid cardiolipin (CL) plays a crucial role in the initiation of apoptosis by catalyzing lipid peroxidation in mitochondrial membranes. In our previous papers, we found that CytC and CL mixed in millimolar concentrations form a sediment showing microcrystals composed of nanospheres (Cyt-CL) of 11-12 and 8 nm in diameter. The hypothesis was proposed that Cyt-CL, having hydrophobic shell, may appear inside the membrane lipid bilayer in mitochondria and peroxidase membrane phospholipids so initiating the apoptotic cascade. In this work, Cyt-CL complex dissolved in chloroform or hexane was investigated as a model of the complex in mitochondrial membranes. We used dynamic light scattering method to measure the size of the particles. The analysis of particles size distribution of Cyt-CL in chloroform allows to reveal three dominant diameters of 12.1 ± 1.4, 7.8 ± 1.0, and 4.7 ± 0.7 nm. The first two values are closed to those, earlier obtained with small-angle X-ray scattering method in Cyt-CL microcrystals, 11.1 ± 1.0 and 8.0 ± 0.7 nm. CL extracted in chloroform-methanol forms a real solution of particles with diameter of 0.7 ± 0.1 nm. In methanol-water phase, CL and CL + CytC mixture form particles of 83.7 ± 9.8 and 71.3 ± 11.6 nm, respectively. Apparently, cardiolipin in 50% methanol forms single-layer liposomes regardless of the presence of CytC in the medium. Partial unfolding of CytC in the complex was evidenced by (a) appearance of fluorescence of tyrosine and tryptophan residues and (b) disappearance of the absorption band at 699 nm due to breakdown of heme iron - methionine bond > F⋯S(Met80). In hydrophobic solvent Cyt-CL exhibited quasi-lipoperoxidase and lipoxygenase activity as was shown in kinetic measurements of chemiluminescence enhanced by coumarin C-525, a selective sensitizer of chemiluminescence, associated with reactions of lipid peroxyl radicals. Our data in this model system do not contradict the hypothesis (Vladimirov, Y.A. et al. Biochemistry (Mosc) 78, 1086-1097) that nanospheres of Cyt-CL complex, embedded into the lipid phase of mitochondrial membrane, catalyze lipid peroxidation, thereby initiating apoptosis.

摘要

线粒体蛋白细胞色素 c (CytC) 与阴离子磷脂心磷脂 (CL) 的复合物在通过催化线粒体膜中的脂质过氧化作用来启动细胞凋亡的过程中起着至关重要的作用。在我们之前的论文中,我们发现 CytC 和 CL 在毫摩尔浓度下混合形成沉淀,该沉淀显示由 11-12 和 8nm 直径的纳米球组成的微晶体。提出了这样的假设,即具有疏水性外壳的 Cyt-CL 可能出现在线粒体的膜脂双层内和过氧化物酶膜磷脂中,从而引发凋亡级联反应。在这项工作中,我们研究了溶解在氯仿或己烷中的 Cyt-CL 复合物作为线粒体膜中复合物的模型。我们使用动态光散射法测量颗粒的大小。对氯仿中 Cyt-CL 颗粒大小分布的分析表明,有三个主要的直径分别为 12.1±1.4nm、7.8±1.0nm 和 4.7±0.7nm。前两个值与用小角度 X 射线散射法在 Cyt-CL 微晶体中获得的值 11.1±1.0nm 和 8.0±0.7nm 接近。从氯仿-甲醇中提取的 CL 形成直径为 0.7±0.1nm 的真实粒子溶液。在甲醇-水相中,CL 和 CL+CytC 混合物分别形成 83.7±9.8nm 和 71.3±11.6nm 的颗粒。显然,无论介质中是否存在 CytC,50%甲醇中的 CL 都会形成单层脂质体。复合物中 CytC 的部分展开通过以下方式得到证实:(a)酪氨酸和色氨酸残基的荧光出现,(b)由于血红素铁-蛋氨酸键的断裂,699nm 处的吸收带消失 > F⋯S(Met80)。在疏水性溶剂中,Cyt-CL 表现出准脂氧合酶和脂加氧酶活性,这可以通过香豆素 C-525 增强的化学发光动力学测量来证明,香豆素 C-525 是化学发光的选择性敏化剂,与脂氧自由基反应有关。在这个模型系统中,我们的数据并不与假说(Vladimirov,Y.A.等人,Biochemistry(Mosc)78,1086-1097)相矛盾,该假说认为 Cyt-CL 复合物的纳米球嵌入线粒体膜的脂质相中,催化脂质过氧化作用,从而引发细胞凋亡。

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