4.3 Article

TMSEG: Novel prediction of transmembrane helices

Journal

PROTEINS-STRUCTURE FUNCTION AND BIOINFORMATICS
Volume 84, Issue 11, Pages 1706-1716

Publisher

WILEY
DOI: 10.1002/prot.25155

Keywords

membrane protein; protein structure prediction; transmembrane helices; -helical integral membrane protein; transmembrane protein prediction; transmembrane helix prediction

Funding

  1. Alexander von Humboldt Foundation
  2. National Institutes of Health (NIH) [U54 GM095315]

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Transmembrane proteins (TMPs) are important drug targets because they are essential for signaling, regulation, and transport. Despite important breakthroughs, experimental structure determination remains challenging for TMPs. Various methods have bridged the gap by predicting transmembrane helices (TMHs), but room for improvement remains. Here, we present TMSEG, a novel method identifying TMPs and accurately predicting their TMHs and their topology. The method combines machine learning with empirical filters. Testing it on a non-redundant dataset of 41 TMPs and 285 soluble proteins, and applying strict performance measures, TMSEG outperformed the state-of-the-art in our hands. TMSEG correctly distinguished helical TMPs from other proteins with a sensitivity of 98 +/- 2% and a false positive rate as low as 3 +/- 1%. Individual TMHs were predicted with a precision of 87 +/- 3% and recall of 84 +/- 3%. Furthermore, in 63 +/- 6% of helical TMPs the placement of all TMHs and their inside/outside topology was correctly predicted. There are two main features that distinguish TMSEG from other methods. First, the errors in finding all helical TMPs in an organism are significantly reduced. For example, in human this leads to 200 and 1600 fewer misclassifications compared to the second and third best method available, and 4400 fewer mistakes than by a simple hydrophobicity-based method. Second, TMSEG provides an add-on improvement for any existing method to benefit from. Proteins 2016; 84:1706-1716. (c) 2016 Wiley Periodicals, Inc.

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