CONFOLD2: Improved contact-driven ab initio protein structure modeling

Authors

Badri Adhikari, University of Missouri-St. Louis, Department of Mathematics and Computer ScienceFollow
Jianlin Cheng, University of Missouri

Document Type

Article

Abstract

Background: Contact-guided protein structure prediction methods are becoming more and more successful because of the latest advances in residue-residue contact prediction. To support contact-driven structure prediction, effective tools that can quickly build tertiary structural models of good quality from predicted contacts need to be developed. Results: We develop an improved contact-driven protein modelling method, CONFOLD2, and study how it may be effectively used for ab initio protein structure prediction with predicted contacts as input. It builds models using various subsets of input contacts to explore the fold space under the guidance of a soft square energy function, and then clusters the models to obtain the top five models. CONFOLD2 obtains an average reconstruction accuracy of 0.57 TM-score for the 150 proteins in the PSICOV contact prediction dataset. When benchmarked on the CASP11 contacts predicted using CONSIP2 and CASP12 contacts predicted using Raptor-X, CONFOLD2 achieves a mean TM-score of 0.41 on both datasets. Conclusion: CONFOLD2 allows to quickly generate top five structural models for a protein sequence when its secondary structures and contacts predictions at hand. The source code of CONFOLD2 is publicly available at https://github.com/multicom-toolbox/CONFOLD2/.

Publication Date

1-25-2018

Publication Title

BMC Bioinformatics

Volume

19

Issue

1

DOI

10.1186/s12859-018-2032-6

Recommended Citation

Adhikari, Badri and Cheng, Jianlin, "CONFOLD2: Improved contact-driven ab initio protein structure modeling" (2018). Computer Science Faculty Works. 5.
DOI: https://doi.org/10.1186/s12859-018-2032-6
Available at: https://irl.umsl.edu/cmpsci-faculty/5