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PRALINETM:一种改进跨膜蛋白多重比对的策略。

PRALINETM: a strategy for improved multiple alignment of transmembrane proteins.

作者信息

Pirovano Walter, Feenstra K Anton, Heringa Jaap

机构信息

Centre for Integrative Bioinformatics VU (IBIVU), VU University Amsterdam, De Boelelaan 1081A, 1081 HV Amsterdam, The Netherlands.

出版信息

Bioinformatics. 2008 Feb 15;24(4):492-7. doi: 10.1093/bioinformatics/btm636. Epub 2008 Jan 2.

Abstract

MOTIVATION

Membrane-bound proteins are a special class of proteins. The regions that insert into the cell-membrane have a profoundly different hydrophobicity pattern compared with soluble proteins. Multiple alignment techniques use scoring schemes tailored for sequences of soluble proteins and are therefore in principle not optimal to align membrane-bound proteins.

RESULTS

Transmembrane (TM) regions in protein sequences can be reliably recognized using state-of-the-art sequence prediction techniques. Furthermore, membrane-specific scoring matrices are available. We have developed a new alignment method, called PRALINETM, which integrates these two features to enhance multiple sequence alignment. We tested our algorithm on the TM alignment benchmark set by Bahr et al. (2001), and showed that the quality of TM alignments can be significantly improved compared with the quality produced by a standard multiple alignment technique. The results clearly indicate that the incorporation of these new elements into current state-of-the-art alignment methods is crucial for optimizing the alignment of TM proteins.

AVAILABILITY

A webserver is available at http://www.ibi.vu.nl/programs/pralinewww.

摘要

动机

膜结合蛋白是一类特殊的蛋白质。与可溶性蛋白相比,插入细胞膜的区域具有截然不同的疏水性模式。多重比对技术使用的评分方案是为可溶性蛋白序列量身定制的,因此原则上并不适合用于比对膜结合蛋白。

结果

利用先进的序列预测技术可以可靠地识别蛋白质序列中的跨膜(TM)区域。此外,还有针对膜的评分矩阵。我们开发了一种新的比对方法,称为PRALINETM,它整合了这两个特性以增强多重序列比对。我们在Bahr等人(2001年)设定的TM比对基准集上测试了我们的算法,结果表明,与标准多重比对技术产生的质量相比,TM比对的质量可以得到显著提高。结果清楚地表明,将这些新元素纳入当前的先进比对方法对于优化TM蛋白的比对至关重要。

可用性

可通过http://www.ibi.vu.nl/programs/pralinewww访问网络服务器。

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