Dynamic heterogeneity in the folding/unfolding transitions of FiP35

Mori, Taro; Saito, Shinji

doi:10.1063/1.4916641

Cited by 22 publications

(32 citation statements)

References 46 publications

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“…The presence of this state shows that folding cannot be downhill incipient, in agreement with other studies. [46][47][48] In addition, there is an additional basin (C) just outside the unfolded state at ψ 1 ≈ 0.007 and a cloud of dispersed states (B) at ψ 1 ≈ 0.004 which elongates orthogonally to the horizontal folding direction. To better investigate the features of these states, heavy atom contact maps were built on sets of structures sampled from the trajectory.…”

Section: Free Energy and Structure Analysismentioning

confidence: 99%

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Investigating Molecular Kinetics by Variationally Optimized Diffusion Maps

Boninsegna

Gobbo

Noé

et al. 2015

J. Chem. Theory Comput.

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Identification of the collective coordinates that describe rare events in complex molecular transitions such as protein folding has been a key challenge in the theoretical molecular sciences. In the Diffusion Map approach, one assumes that the molecular configurations sampled have been generated by a diffusion process, and one uses the eigenfunctions of the corresponding diffusion operator as reaction coordinates. While diffusion coordinates (DCs) appear to provide a good approximation to the true dynamical reaction coordinates, they are not parametrized using dynamical information. Thus, their approximation quality could not, as yet, be validated, nor could the diffusion map eigenvalues be used to compute relaxation rate constants of the system. Here we combine the Diffusion Map approach with the recently proposed Variational Approach for Conformation Dynamics (VAC). Diffusion Map coordinates are used as a basis set, and their optimal linear combination is sought using the VAC, which employs time-correlation information on the molecular dynamics (MD) trajectories. We have applied this approach to ultra-long MD simulations of the Fip35 WW domain and found that the first DCs are indeed a good approximation to the true reaction coordinates of the system, but they could be further improved using the VAC. Using the Diffusion Map basis, excellent approximations to the relaxation rates of the system are obtained. Finally, we evaluate the quality of different metric spaces and find that pairwise minimal root-mean-square deviation performs poorly, while operating in the recently introduced kinetic maps based on the time-lagged independent component analysis gives the best performance.

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Section: Free Energy and Structure Analysismentioning

confidence: 99%

“…Thus, state B represents a misfolded state, similar to those found in previous studies. 47,48 Finally, state (C) exhibits a random-coil structure, where the second hairpin starts being formed (a number of key contacts are being formed). Projecting productive trajectory portions onto the free energy plot in Fig.…”

Section: Free Energy and Structure Analysismentioning

confidence: 99%

Investigating Molecular Kinetics by Variationally Optimized Diffusion Maps

Boninsegna

Gobbo

Noé

et al. 2015

J. Chem. Theory Comput.

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“…Indeed, characteristics of the glass-transition physics like cooperative motions called dynamic heterogeneities were reported to be generated during the motion of various motors [38][39][40][41][42]. The photo-fluidization and softening of the host material, or transient liquid-like behaviors, were also reported by different groups experimentally and by simulations [38,[43][44][45][46] with particular motors.…”

Section: Introductionmentioning

confidence: 87%

Folding time dependence of the motions of a molecular motor in an amorphous medium

et al. 2017

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We investigate the dependence of the displacements of a molecular motor embedded inside a glassy material on its folding characteristic time τ f . We observe two different time regimes. For slow foldings (regime I) the diffusion evolves very slowly with τ f , while for rapid foldings (regime II) the diffusion increases strongly with τ f ( D ≈ τ −2 f ) suggesting two different physical mechanisms. We find that in regime I the motor's displacement during the folding process is counteracted by a reverse displacement during the unfolding, while in regime II this counteraction is much weaker. We notice that regime I behavior is reminiscent of the scallop theorem that holds for larger motors in a continuous medium. We find that the difference in the efficiency of the motor's motion explains most of the observed difference between the two regimes. For fast foldings the motor trajectories differ significantly from the opposite trajectories induced by the following unfolding process, resulting in a more efficient global motion than for slow foldings. This result agrees with the fluctuation theorems expectation for time reversal mechanisms. In agreement with the fluctuation theorems we find that the motors are unexpectedly more efficient when they are generating more entropy, a result that can be used to increase dramatically the motor's motion.

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“…(Here, dynamic analysis methods mean that the variations of physical quantities with time are directly used in analysis.) Accordingly, many methods have been developed to analyze the dynamics and kinetics of protein simulations [47][48][49][50][51][52][53][54][55]. The Markov state model has been reported and applied to many protein systems [49,52,53,[56][57][58][59][60][61][62][63][64][65][66][67][68]; it can analyze transitions between local minimum-energy states, which are identified by using clustering analysis methods.…”

mentioning

confidence: 99%

“…developed for molecular simulations of biopolymer systems. In these techniques, such as time structure-based independent component analysis (tICA) [50,51], time-lagged independent component analysis (TICA) [52,53], and dynamic component analysis (DCA) [54,55], time correlation matrices of certain physical quantities or states are used. Notably, tICA is a special case of RMA with t 0 =0, and gave rise to a different concept, the independent component analysis, to RMA with t 0 =0.…”

mentioning

confidence: 99%

Analysis of molecular dynamics simulations of 10-residue peptide, chignolin, using statistical mechanics: Relaxation mode analysis and three-dimensional reference interaction site model theory

2019

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Molecular dynamics simulation is a fruitful tool for investigating the structural stability, dynamics, and functions of biopolymers at an atomic level. In recent years, simulations can be performed on time scales of the order of milliseconds using specialpurpose systems. Since the most stable structure, as well as meta-stable structures and intermediate structures, is included in trajectories in long simulations, it is necessary to develop analysis methods for extracting them from trajectories of simulations. For these structures, methods for evaluating the stabilities, including the solvent effect, are also needed. We have developed relaxation mode analysis to investigate dynamics and kinetics of simulations based on statistical mechanics. We have also applied the three-dimensional reference interaction site model theory to investigate stabilities with solvent effects. In this paper, we review the results for designing amino-acid substitution of the 10-residue peptide, chignolin, to stabilize the misfolded structure using these developed analysis methods.It is important to develop analysis methods for molecular simulations of protein systems. We have developed relaxation mode analysis to investigate dynamics and kinetics of simulations. We also have applied the three-dimensional reference interaction site model theory to investigate stability with solvent effects. Here, we review the results for designing amino-acid substitution of 10-residue peptide, chignolin, to stabilize the misfolded structure using these analysis methods based on statistical mechanics. Background of mode decomposition methods for protein simulationsAs longer and larger MD simulations are performed, it has become increasingly important to develop methods to extract the "essential" information from the trajectory. The reduction in the large number of degrees of freedom of coordinates to a few collective ones is an active field of theo retical research. In NMA, the normal modes near the minimum potential energy of the protein molecule are obtained [3,24,25]. LMA investigates modes around a minimumenergy state, including the water effect [4,6,26,27]. An elastic network model and a Gaussian network model approximately calculate normal modes with large amplitudes by using the harmonic potential of coarse-grained models [28][29][30][31][32]. This method extracts collective modes with large amplitudes for large protein systems like viruses, because such proteins have rigid-like motions [33]. PCA, also called quasiharmonic analysis or the essential dynamics method [6,7,[34][35][36][37][38], is one of the most popular methods for analyzing the structural fluctuations around the average structure. The modes with large structure fluctuations are extracted and are considered cooperative movement, and the relation of these fluctuations with function has been widely examined. The obtained modes are also used as the axis of the free-energy surface. The JAM model was introduced for treating multiple-hierarchy free-energy landscapes [9]. They divided protei...

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Dynamic heterogeneity in the folding/unfolding transitions of FiP35

Cited by 22 publications

References 46 publications

Investigating Molecular Kinetics by Variationally Optimized Diffusion Maps

Investigating Molecular Kinetics by Variationally Optimized Diffusion Maps

Folding time dependence of the motions of a molecular motor in an amorphous medium

Analysis of molecular dynamics simulations of 10-residue peptide, chignolin, using statistical mechanics: Relaxation mode analysis and three-dimensional reference interaction site model theory

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