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首页> 外文期刊>FEBS Open Bio >In silico prediction of a disease-associated STIL mutant and its affect on the recruitment of centromere protein J (CENPJ)
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In silico prediction of a disease-associated STIL mutant and its affect on the recruitment of centromere protein J (CENPJ)

机译:在计算机上预测与疾病相关的STIL突变体及其对着丝粒蛋白J(CENPJ)募集的影响

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Human STIL (SCL/TAL1 interrupting locus) protein maintains centriole stability and spindle pole localisation. It helps in recruitment of CENPJ (Centromere protein J)/CPAP (centrosomal P4.1-associated protein) and other centrosomal proteins. Mutations in STIL protein are reported in several disorders, especially in deregulation of cell cycle cascades. In this work, we examined the non-synonymous single nucleotide polymorphisms (nsSNPs) reported in STIL protein for their disease association. Different SNP prediction tools were used to predict disease-associated nsSNPs. Our evaluation technique predicted rs147744459 (R242C) as a highly deleterious disease-associated nsSNP and its interaction behaviour with CENPJ protein. Molecular modelling, docking and molecular dynamics simulation were conducted to examine the structural consequences of the predicted disease-associated mutation. By molecular dynamic simulation we observed structural consequences of R242C mutation which affects interaction of STIL and CENPJ functional domains. The result obtained in this study will provide a biophysical insight into future investigations of pathological nsSNPs using a computational platform.
机译:人STIL(SCL / TAL1中断基因座)蛋白可维持中心粒稳定性和纺锤体极点定位。它有助于募集CENPJ(Centromere蛋白J)/ CPAP(中心体P4.1相关蛋白)和其他中心体蛋白。在几种疾病中,特别是在细胞周期级联失调中,报道了STIL蛋白的突变。在这项工作中,我们检查了STIL蛋白中报告的与疾病相关的非同义单核苷酸多态性(nsSNPs)。使用了不同的SNP预测工具来预测与疾病相关的nsSNP。我们的评估技术将rs147744459(R242C)预测为高度有害的疾病相关nsSNP及其与CENPJ蛋白的相互作用。进行了分子建模,对接和分子动力学模拟,以检查预测的疾病相关突变的结构后果。通过分子动力学模拟,我们观察到R242C突变的结构后果,该突变影响STIL和CENPJ功能域的相互作用。这项研究中获得的结果将为使用计算平台对病理nsSNPs的未来研究提供生物物理学的见识。

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