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HMM_RA: An Improved Method for Alpha-Helical Transmembrane Protein Topology Prediction

机译:HMM_RA:一种用于α-螺旋跨膜蛋白拓扑预测的改进方法

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摘要

α-helical transmembrane (TM) proteins play important and diverse functional roles in cells. The ability to predict the topology of these proteins is important for identifying functional sites and inferring function of membrane proteins. This paper presents a Hidden Markov Model (referred to as HMM_RA) that can predict the topology of α-helical transmembrane proteins with improved performance. HMM_RA adopts the same structure as the HMMTOP method, which has five modules: inside loop, inside helix tail, membrane helix, outside helix tail and outside loop. Each module consists of one or multiple states. HMM_RA allows using reduced alphabets to encode protein sequences. Thus, each state of HMM_RA is associated with n emission probabilities, where n is the size of the reduced alphabet set. Direct comparisons using two standard data sets show that HMM_RA consistently outperforms HMMTOP and TMHMM in topology prediction. Specifically, on a high-quality data set of 83 proteins, HMM_RA outperforms HMMTOP by up to 7.6% in topology accuracy and 6.4% in α-helices location accuracy. On the same data set, HMM_RA outperforms TMHMM by up to 6.4% in topology accuracy and 2.9% in location accuracy. Comparison also shows that HMM_RA achieves comparable performance as Phobius, a recently published method.
机译:α-螺旋跨膜(TM)蛋白在细胞中起着重要而多样的功能作用。预测这些蛋白质的拓扑结构的能力对于鉴定功能位点和推断膜蛋白的功能很重要。本文提出了一种隐马尔可夫模型(称为HMM_RA),该模型可以预测具有改进性能的α螺旋跨膜蛋白的拓扑。 HMM_RA采用与HMMTOP方法相同的结构,该方法具有五个模块:内部循环,内部螺旋尾部,膜螺旋,外部螺旋尾部和外部循环。每个模块由一个或多个状态组成。 HMM_RA允许使用缩略字母来编码蛋白质序列。因此,HMM_RA的每个状态都与n个发射概率相关联,其中n是精简字母集的大小。使用两个标准数据集的直接比较表明,HMM_RA在拓扑预测中始终优于HMMTOP和TMHMM。具体而言,在包含83种蛋白质的高质量数据集上,HMM_RA在拓扑准确度方面优于HMMTOP方面,在α螺旋位置准确性方面优于6.4%。在相同的数据集上,HMM_RA在拓扑精度和位置精度方面均比TMHMM高出6.4%。比较还表明,HMM_RA的性能与最近发布的方法Phobius相当。

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