United-residue force field for off-lattice protein-structure simulations: III. Origin of backbone hydrogen-bonding cooperativity in united-residue potentials

Liwo, Adam; Kaźmierkiewicz, Rajmund; Czaplewski, Cezary; Groth, Małgorzata; Ołdziej, Stanisław; Wawak, Ryszard J.; Rackovsky, S.; Pincus, Matthew R.; Scheraga, Harold A.

doi:10.1002/(sici)1096-987x(199802)19:3<259::aid-jcc1>3.0.co;2-s

Cited by 163 publications

(313 citation statements)

References 26 publications

(22 reference statements)

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“…Employing the identity in eq (36), it can be proven that (38) Let i and j correspond to CG site types α and β, respectively, and define the radial distribution function (39) then (40) In the case that α = β, the two terms in the summations are equivalent and the result simplifies: (41) A more detailed derivation is provided in the supporting information section.…”

Section: Discussionmentioning

confidence: 99%

Multiscale Coarse-Graining and Structural Correlations: Connections to Liquid-State Theory

et al. 2007

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(2005)]. If no approximations are made, the MS-CG method yields a many-body multi-dimensional potential of mean force describing the interactions between CG sites. However, numerical applications of the MS-CG method typically employ a set of pair potentials to describe non-bonded interactions. The analogy between coarse-graining and the inverse problem of liquid state theory clarifies the general significance of three-particle correlations for the development of such CG pair potentials. It is demonstrated that the MS-CG methodology incorporates critical three-body correlation effects and that, for isotropic homogeneous systems evolving under a central pair potential, the MS-CG equations are a discretized representation of the well-known Yvon-Born-Green equation. Numerical calculations validate the theory and illustrate the role of these structural correlations in the MS-CG method.

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Section: Discussionmentioning

confidence: 99%

Multiscale Coarse-Graining and Structural Correlations: Connections to Liquid-State Theory

et al. 2007

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“…The RFE is defined as the free energy of a given coarse-grain conformation obtained by integrating the Boltzmann factor of the all-atom (i.e., the polypeptide chain plus solvent) energy over the degrees of freedom that are neglected in the united-residue model. 38,40,45,46 The complete UNRES potential-energy function is expressed by eq 1. The terms U SC i SC j correspond to the mean free energy of hydrophobic (hydrophilic) interactions between the side chains.…”

Section: United-residue Force Fieldmentioning

confidence: 99%

“…with (38) where the matrix G is defined by eq 26, μ i , i = 1, 2, …, n are the eigenvalues of G, and V is the matrix of the eigenvectors of G. The velocities expressed in normal coordinates (ξ 1 , ξ 2 , …, ξ n ) can now be sampled from normal distributions, and the initial velocities q˙ of the virtualbond vectors can be computed by inverting eq 38, as expressed by eqs 39 and 40, respectively.…”

Section: Generating Initial Velocitiesmentioning

confidence: 99%

Molecular Dynamics with the United-Residue Model of Polypeptide Chains. I. Lagrange Equations of Motion and Tests of Numerical Stability in the Microcanonical Mode

et al. 2005

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The Lagrange formalism was implemented to derive the equations of motion for the physics-based united-residue (UNRES) force field developed in our laboratory. The C α… C α and C α… SC (SC denoting a side-chain center) virtual-bond vectors were chosen as variables. The velocity Verlet algorithm was adopted to integrate the equations of motion. Tests on the unblocked Ala 10 polypeptide showed that the algorithm is stable in short periods of time up to the time step of 1.467 fs; however, even with the shorter time step of 0.489 fs, some drift of the total energy occurs because of momentary jumps of the acceleration. These jumps are caused by numerical instability of the forces arising from the U rot component of UNRES that describes the energetics of side-chain-rotameric states. Test runs on the Gly 10 sequence (in which U rot is not present) and on the Ala 10 sequence with U rot replaced by a simple numerically stable harmonic potential confirmed this observation; oscillations of the total energy were observed only up to the time step of 7.335 fs, and some drift in the total energy or instability of the trajectories started to appear in long-time (2 ns and longer) trajectories only for the time step of 9.78 fs. These results demonstrate that the present U rot components (which are statistical potentials derived from the Protein Data Bank) must be replaced with more numerically stable functions; this work is under way in our laboratory. For the purpose of our present work, a nonsymplectic variable-time-step algorithm was introduced to reduce the energy drift for regular polypeptide sequences. The algorithm scales down the time step at a given point of a trajectory if the maximum change of acceleration exceeds a selected cutoff value. With this algorithm, the total energy is reasonably conserved up to a time step of 2.445 fs, as tested on the unblocked Ala 10 polypeptide. We also tried a symplectic multiple-time-step reversible RESPA algorithm and achieved satisfactory energy conservation for time steps up to 7.335 fs. However, at present, it appears that the reversible RESPA algorithm is several times more expensive than the variable-time-step algorithm because of the necessity to perform additional matrix multiplications. We also observed that, because Ala 10 folds and unfolds within picoseconds in the microcanonical mode, this suggests that the effective (event-based) time unit in UNRES dynamics is much larger than that of all-atom dynamics because of averaging over the fast-moving degrees of freedom in deriving the UNRES potential.

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“…By reducing the number of degrees of freedom, coarse-grained models of proteins can drastically reduce the intrinsic cost of simulating a time step, as well as increasing the duration of each step. The strategy has been pursued for many different problems over the years from protein folding to aggregation to conformational change (8,(15)(16)(17)(18)(19)(20)(21)(22)(23)(24)(25)(26)(27). Although coarse-grained models fail to capture atomistic detail and may have limited biochemical accuracy, recent work may permit the use of simplified ensembles in accelerating atomistic sampling (28,29).…”

mentioning

confidence: 99%

Efficient and verified simulation of a path ensemble for conformational change in a united-residue model of calmodulin

Zhang

Jasnow

Zuckerman

2007

Proc. Natl. Acad. Sci. U.S.A.

120

163

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The computational sampling of rare, large-scale, conformational transitions in proteins is a well appreciated challenge-for which a number of potentially efficient path-sampling methodologies have been proposed. Here, we study a large-scale transition in a united-residue model of calmodulin using the ''weighted ensemble'' (WE) approach of Huber and Kim. Because of the model's relative simplicity, we are able to compare our results with bruteforce simulations. The comparison indicates that the WE approach quantitatively reproduces the brute-force results, as assessed by considering (i) the reaction rate, (ii) the distribution of event durations, and (iii) structural distributions describing the heterogeneity of the paths. Importantly, the WE method is readily applied to more chemically accurate models, and by studying a series of lower temperatures, our results suggest that the WE method can increase efficiency by orders of magnitude in more challenging systems.transition path ͉ path sampling ͉ weighted ensemble ͉ conformational transition

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United-residue force field for off-lattice protein-structure simulations: III. Origin of backbone hydrogen-bonding cooperativity in united-residue potentials

Cited by 163 publications

References 26 publications

Multiscale Coarse-Graining and Structural Correlations: Connections to Liquid-State Theory

Multiscale Coarse-Graining and Structural Correlations: Connections to Liquid-State Theory

Molecular Dynamics with the United-Residue Model of Polypeptide Chains. I. Lagrange Equations of Motion and Tests of Numerical Stability in the Microcanonical Mode

Efficient and verified simulation of a path ensemble for conformational change in a united-residue model of calmodulin

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