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Computational Methods for Predicting Structure of Membrane Proteins Using Amino Acid Sequences

机译:使用氨基酸序列预测膜蛋白结构的计算方法

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The structure of membrane proteins specifies their functional properties, which are important for medicine and pharmacology and, therefore, is of significant interest. The repetition of transmembrane regions that consist of hydrophobic amino acids is a characteristic and organic feature of polytopic membrane proteins. The ordered repetition (periodicity) can be detected by the Fourier method applied to a digital image of the symbolic amino acid sequence of a protein. In the present work, this investigation was carried out for 24 transmembrane proteins (successfully for 14 of them). If the repetition of transmembrane regions is aperiodic, it can be revealed by another method, that is, the method of the reiterated (four to five times) averaging of the protein hydrophobicity function in a window within the limits of 9-11 amino acids that moves along the sequence. This novel method was apphed to the 24 transmembrane proteins (successfully for 19 of them) and demonstrated higher suitability than the Fourier method for predicting the secondary structure of these proteins and the corresponding functional properties.
机译:膜蛋白的结构决定了它们的功能特性,这对医学和药理学很重要,因此引起了极大的兴趣。由疏水性氨基酸组成的跨膜区域的重复是多位膜蛋白的特征和有机特征。可以通过将傅立叶方法应用于蛋白质的符号氨基酸序列的数字图像来检测有序重复(周期性)。在目前的工作中,对24种跨膜蛋白(其中14种成功)进行了这项研究。如果跨膜区域的重复是非周期性的,则可以通过另一种方法来揭示,即在9-11个氨基酸的范围内,重复(四到五次)平均化窗口中蛋白质疏水功能的方法,沿着序列移动。这种新方法适用于24种跨膜蛋白(其中19种成功),并且比傅里叶法预测这些蛋白的二级结构和相应的功能特性具有更高的适用性。

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