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对螺旋跨膜蛋白的拓扑结构预测准确率达86%。

Topology prediction for helical transmembrane proteins at 86% accuracy.

作者信息

Rost B, Fariselli P, Casadio R

机构信息

European Molecular Biology Laboratory, Heidelberg, Germany.

出版信息

Protein Sci. 1996 Aug;5(8):1704-18. doi: 10.1002/pro.5560050824.

Abstract

Previously, we introduced a neural network system predicting locations of transmembrane helices (HTMs) based on evolutionary profiles (PHDhtm, Rost B, Casadio R, Fariselli P, Sander C, 1995, Protein Sci 4:521-533). Here, we describe an improvement and an extension of that system. The improvement is achieved by a dynamic programming-like algorithm that optimizes helices compatible with the neural network output. The extension is the prediction of topology (orientation of first loop region with respect to membrane) by applying to the refined prediction the observation that positively charged residues are more abundant in extra-cytoplasmic regions. Furthermore, we introduce a method to reduce the number of false positives, i.e., proteins falsely predicted with membrane helices. The evaluation of prediction accuracy is based on a cross-validation and a double-blind test set (in total 131 proteins). The final method appears to be more accurate than other methods published: (1) For almost 89% (+/-3%) of the test proteins, all HTMs are predicted correctly. (2) For more than 86% (+/-3%) of the proteins, topology is predicted correctly. (3) We define reliability indices that correlate with prediction accuracy: for one half of the proteins, segment accuracy raises to 98%; and for two-thirds, accuracy of topology prediction is 95%. (4) The rate of proteins for which HTMs are predicted falsely is below 2% (+/-1%). Finally, the method is applied to 1,616 sequences of Haemophilus influenzae. We predict 19% of the genome sequences to contain one or more HTMs. This appears to be lower than what we predicted previously for the yeast VIII chromosome (about 25%).

摘要

此前,我们介绍了一种基于进化轮廓预测跨膜螺旋(HTM)位置的神经网络系统(PHDhtm,罗斯特B,卡萨迪奥R,法里塞利P,桑德C,1995年,《蛋白质科学》4:521 - 533)。在此,我们描述该系统的改进与扩展。改进通过一种类似动态规划的算法实现,该算法优化与神经网络输出兼容的螺旋。扩展是通过将带正电荷残基在胞外区域更丰富这一观察结果应用于优化后的预测来预测拓扑结构(第一个环区相对于膜的方向)。此外,我们引入了一种减少假阳性数量的方法,即错误预测带有膜螺旋的蛋白质。预测准确性的评估基于交叉验证和一个双盲测试集(总共131种蛋白质)。最终方法似乎比已发表的其他方法更准确:(1)对于近89%(±3%)的测试蛋白质,所有HTM均被正确预测。(2)对于超过86%(±3%)的蛋白质,拓扑结构被正确预测。(3)我们定义了与预测准确性相关的可靠性指标:对于一半的蛋白质,片段准确性提高到98%;对于三分之二的蛋白质,拓扑预测准确性为95%。(4)被错误预测带有HTM的蛋白质比例低于2%(±1%)。最后,该方法应用于流感嗜血杆菌的1616个序列。我们预测19%的基因组序列含有一个或多个HTM。这似乎低于我们之前对酵母VIII号染色体的预测(约25%)。

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