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Use of mutual information arrays to predict coevolving sites in the full length HIV gp120 protein for subtypes B and C

机译:使用互信息阵列以预测亚型B和C的全长HIV GP120蛋白中的共用部位

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摘要

It is well established that different sites within a protein evolve at different rates according to their role within the protein; identification of these correlated mutations can aid in tasks such as ab initio protein structure, structure function analysis or sequence alignment. Mutual Information is a standard measure for coevolution between two sites but its application is limited by signal to noise ratio. In this work we report a preliminary study to investigate whether larger sequence sets could circumvent this problem by calculating mutual information arrays for two sets of drug naïve sequences from the HIV gp120 protein for the B and C subtypes. Our results suggest that while the larger sequences sets can improve the signal to noise ratio, the gain is offset by the high mutation rate of the HIV virus which makes it more difficult to achieve consistent alignments. Nevertheless, we were able to predict a number of coevolving sites that were supported by previous experimental studies as well as a region close to the C terminal of the protein that was highly variable in the C subtype but highly conserved in the B subtype.
机译:很好地确定,蛋白质中的不同位点根据蛋白质内的作用以不同的速率发展;鉴定这些相关突变可以帮助诸如AB初始蛋白质结构,结构函数分析或序列对准的任务。相互信息是两个站点之间的参与的标准度量,但其应用受到信噪比的限制。在这项工作中,我们报告了一种初步研究,以研究较大的序列组是否可以通过计算来自B和C亚型的HIV GP120蛋白的两组药物Naïve序列来规避这个问题。我们的研究结果表明,虽然较大的序列集可以提高信噪比,但增益由HIV病毒的高突变率偏移,这使得难以实现一致的对准。然而,我们能够预测以前的实验研究支持的许多辅助部位,以及靠近蛋白质的C末端的区域,其在C亚型中具有高度可变的蛋白质,但在B亚型中高度保守。

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