16,232 research outputs found
CLP-based protein fragment assembly
The paper investigates a novel approach, based on Constraint Logic
Programming (CLP), to predict the 3D conformation of a protein via fragments
assembly. The fragments are extracted by a preprocessor-also developed for this
work- from a database of known protein structures that clusters and classifies
the fragments according to similarity and frequency. The problem of assembling
fragments into a complete conformation is mapped to a constraint solving
problem and solved using CLP. The constraint-based model uses a medium
discretization degree Ca-side chain centroid protein model that offers
efficiency and a good approximation for space filling. The approach adapts
existing energy models to the protein representation used and applies a large
neighboring search strategy. The results shows the feasibility and efficiency
of the method. The declarative nature of the solution allows to include future
extensions, e.g., different size fragments for better accuracy.Comment: special issue dedicated to ICLP 201
A Hybrid Monte Carlo Ant Colony Optimization Approach for Protein Structure Prediction in the HP Model
The hydrophobic-polar (HP) model has been widely studied in the field of
protein structure prediction (PSP) both for theoretical purposes and as a
benchmark for new optimization strategies. In this work we introduce a new
heuristics based on Ant Colony Optimization (ACO) and Markov Chain Monte Carlo
(MCMC) that we called Hybrid Monte Carlo Ant Colony Optimization (HMCACO). We
describe this method and compare results obtained on well known HP instances in
the 3 dimensional cubic lattice to those obtained with standard ACO and
Simulated Annealing (SA). All methods were implemented using an unconstrained
neighborhood and a modified objective function to prevent the creation of
overlapping walks. Results show that our methods perform better than the other
heuristics in all benchmark instances.Comment: In Proceedings Wivace 2013, arXiv:1309.712
CPSP-tools – Exact and complete algorithms for high-throughput 3D lattice protein studies
<p>Abstract</p> <p>Background</p> <p>The principles of protein folding and evolution pose problems of very high inherent complexity. Often these problems are tackled using simplified protein models, e.g. lattice proteins. The CPSP-tools package provides programs to solve exactly and completely the problems typical of studies using 3D lattice protein models. Among the tasks addressed are the prediction of (all) globally optimal and/or suboptimal structures as well as sequence design and neutral network exploration.</p> <p>Results</p> <p>In contrast to stochastic approaches, which are not capable of answering many fundamental questions, our methods are based on fast, non-heuristic techniques. The resulting tools are designed for high-throughput studies of 3D-lattice proteins utilising the Hydrophobic-Polar (HP) model. The source bundle is freely available <abbrgrp><abbr bid="B1">1</abbr></abbrgrp>.</p> <p>Conclusion</p> <p>The CPSP-tools package is the first set of exact and complete methods for extensive, high-throughput studies of non-restricted 3D-lattice protein models. In particular, our package deals with cubic and face centered cubic (FCC) lattices.</p
Paradigms for computational nucleic acid design
The design of DNA and RNA sequences is critical for many endeavors, from DNA nanotechnology, to PCR‐based applications, to DNA hybridization arrays. Results in the literature rely on a wide variety of design criteria adapted to the particular requirements of each application. Using an extensively studied thermodynamic model, we perform a detailed study of several criteria for designing sequences intended to adopt a target secondary structure. We conclude that superior design methods should explicitly implement both a positive design paradigm (optimize affinity for the target structure) and a negative design paradigm (optimize specificity for the target structure). The commonly used approaches of sequence symmetry minimization and minimum free‐energy satisfaction primarily implement negative design and can be strengthened by introducing a positive design component. Surprisingly, our findings hold for a wide range of secondary structures and are robust to modest perturbation of the thermodynamic parameters used for evaluating sequence quality, suggesting the feasibility and ongoing utility of a unified approach to nucleic acid design as parameter sets are refined further. Finally, we observe that designing for thermodynamic stability does not determine folding kinetics, emphasizing the opportunity for extending design criteria to target kinetic features of the energy landscape
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