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“Pinning strategy”: a novel approach for predicting the backbone structure in terms of protein blocks from sequence

机译:“定位策略”:一种根据序列中的蛋白质块预测骨架结构的新方法

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The description of protein 3D structures can be performed through a library of 3D fragments, named a structural alphabet. Our structural alphabet is composed of 16 small protein fragments of 5 Cα in length, called protein blocks (PBs). It allows an efficient approximation of the 3D protein structures and a correct prediction of the local structure. The 72 most frequent series of 5 consecutive PBs, called structural words (SWs) are able to cover more than 90% of the 3D structures. PBs are highly conditioned by the presence of a limited number of transitions between them. In this study, we propose a new method called “pinning strategy” that used this specific feature to predict long protein fragments. Its goal is to define highly probable successions of PBs. It starts from the most probable SW and is then extended with overlapping SWs. Starting from an initial prediction rate of 34.4%, the use of the SWs instead of the PBs allows a gain of 4.5%. The pinning strategy simply applied to the SWs increases the prediction accuracy to 39.9%. In a second step, the sequence-structure relationship is optimized, the prediction accuracy reaches 43.6%.
机译:可以通过名为结构字母的3D片段库对蛋白质3D结构进行描述。我们的结构字母由16个长度为5Cα的小蛋白质片段组成,称为蛋白质块(PB)。它允许3D蛋白质结构的有效近似和局部结构的正确预测。 5个连续PB的72个最常见的系列(称为结构词(SW))能够覆盖90%以上的3D结构。 PB受它们之间有限数量的转换的高度限制。在这项研究中,我们提出了一种称为“固定策略”的新方法,该方法使用此特定功能来预测长蛋白片段。其目标是定义PB的高度可能的继承。它从最可能的软件开始,然后通过重叠的软件进行扩展。从34.4%的初始预测率开始,使用SW而不是PB可以提高4.5%。简单地应用于SW的固定策略会将预测准确性提高到39.9%。第二步,优化序列-结构关系,预测精度达到43.6%。

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