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Prediction of localization and interactions of apoptotic proteins

机译:预测凋亡蛋白的定位和相互作用

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摘要

During apoptosis several mitochondrial proteins are released. Some of them participate in caspase-independent nuclear DNA degradation, especially apoptosis-inducing factor (AIF) and endonuclease G (endoG). Another interesting protein, which was expected to act similarly as AIF due to the high sequence homology with AIF is AIF-homologous mitochondrion-associated inducer of death (AMID). We studied the structure, cellular localization, and interactions of several proteins in silico and also in cells using fluorescent microscopy. We found the AMID protein to be cytoplasmic, most probably incorporated into the cytoplasmic side of the lipid membranes. Bioinformatic predictions were conducted to analyze the interactions of the studied proteins with each other and with other possible partners. We conducted molecular modeling of proteins with unknown 3D structures. These models were then refined by MolProbity server and employed in molecular docking simulations of interactions. Our results show data acquired using a combination of modern in silico methods and image analysis to understand the localization, interactions and functions of proteins AMID, AIF, endonuclease G, and other apoptosis-related proteins.
机译:在细胞凋亡期间,释放了几种线粒体蛋白。其中一些参与不依赖胱天蛋白酶的核DNA降解,特别是凋亡诱导因子(AIF)和核酸内切酶G(endoG)。由于与AIF的高序列同源性,另一个与AIF相似的有趣蛋白质是AIF同源线粒体相关的死亡诱导物(AMID)。我们使用荧光显微镜研究了硅蛋白以及细胞中几种蛋白质的结构,细胞定位和相互作用。我们发现AMID蛋白是细胞质的,最有可能整合到脂质膜的细胞质侧。进行了生物信息学预测,以分析研究的蛋白质彼此之间以及与其他可能的伴侣之间的相互作用。我们对未知3D结构的蛋白质进行了分子建模。然后,这些模型由MolProbity服务器进行完善,并用于相互作用的分子对接模拟。我们的结果表明,使用现代计算机技术和图像分析相结合获得的数据可了解蛋白质AMID,AIF,核酸内切酶G和其他与细胞凋亡相关的蛋白质的定位,相互作用和功能。

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