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膜蛋白预测的最新技术。

State-of-the-art in membrane protein prediction.

作者信息

Chen Chien Peter, Rost Burkhard

机构信息

CUBIC, Department of Biochemistry and Molecular Biophysics, Columbia University, New York, NY, USA.

出版信息

Appl Bioinformatics. 2002;1(1):21-35.

Abstract

Membrane proteins are crucial for many biological functions and have become attractive targets for pharmacological agents. About 10%-30% of all proteins contain membrane-spanning helices. Despite recent successes, high-resolution structures for membrane proteins remain exceptional. The gap between known sequences and known structures calls for finding solutions through bioinformatics. While many methods predict membrane helices, very few predict membrane strands. The good news is that most methods for helical membrane proteins are available and are more often right than wrong. The best current prediction methods appear to correctly predict all membrane helices for about 50%-70% of all proteins, and to falsely predict membrane helices for about 10% of all globular proteins. The bad news is that developers have seriously overestimated the accuracy of their methods. In particular, while simple hydrophobicity scales identify many membrane helices, they frequently and incorrectly predict membrane helices in globular proteins. Additionally, all methods tend to confuse signal peptides with membrane helices. Nonetheless, wet-lab biologists can reach into an impressive toolbox for membrane protein predictions. However, the computational biologists will have to improve their methods considerably before they reach the levels of accuracy they claim.

摘要

膜蛋白对许多生物学功能至关重要,已成为药物的诱人靶点。所有蛋白质中约10% - 30%含有跨膜螺旋。尽管最近取得了一些成功,但膜蛋白的高分辨率结构仍然很少见。已知序列与已知结构之间的差距需要通过生物信息学来寻找解决方案。虽然有许多方法可以预测膜螺旋,但预测膜链的方法却很少。好消息是,大多数用于螺旋膜蛋白的方法都有,而且正确的时候比错误的时候多。目前最好的预测方法似乎能正确预测约50% - 70%的所有蛋白质中的所有膜螺旋,而在所有球状蛋白质中错误预测膜螺旋的比例约为10%。坏消息是,开发者严重高估了他们方法的准确性。特别是,虽然简单的疏水性标度能识别许多膜螺旋,但它们经常错误地预测球状蛋白质中的膜螺旋。此外,所有方法都容易将信号肽与膜螺旋混淆。尽管如此,湿实验室生物学家可以使用一个令人印象深刻的膜蛋白预测工具箱。然而,计算生物学家在达到他们所宣称的准确性水平之前,还必须大幅改进他们的方法。

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