Deciphering the Mechanism of Inhibition of SERCA1a by Sarcolipin Using Molecular Simulations

SERCA1a is an ATPase calcium pump that transports Ca2+ from the cytoplasm to the sarco/endoplasmic reticulum lumen. Sarcolipin (SLN), a transmembrane peptide, regulates the activity of SERCA1a by decreasing its Ca2+ transport rate, but its mechanism of action is still not well-understood. To decipher this mechanism, we have performed normal mode analysis in the all-atom model, with the SERCA1a-SLN complex, or the isolated SERCA1a, embedded in an explicit membrane. The comparison of the results allowed us to provide an explanation at the atomic level for the action of SLN that is in good agreement with experimental observations. In our analyses, the presence of SLN locally perturbs the TM6 transmembrane helix and as a consequence modifies the position of D800, one of the key metal-chelating residues. Additionally, it reduces the flexibility of the gating residues, V304, and E309 in TM4, at the entrance of the Ca2+ binding sites, which would decrease the affinity for Ca2+. Unexpectedly, SLN has also an effect on the ATP binding site more than 35 Å away, due to the straightening of TM5, a long helix considered as the spine of the protein. The straightening of TM5 modifies the structure of the P-N linker that sits above it, and which comprises the 351DKTG354 conserved motif, resulting in an increase of the distance between ATP and the phosphorylation site. As a consequence, the turn-over rate could be affected. All this gives SERCA1a the propensity to go toward a Ca2+ low-affinity E2-like state in the presence of SLN and toward a Ca2+ high-affinity E1-like state in the absence of SLN. In addition to a general mechanism of inhibition of SERCA1a regulatory peptides, this study also provides an insight into the conformational transition between the E2 and E1 states.

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Deciphering the mechanism of inhibition of SERCA1a by sarcolipin using molecular simulations

10.1101/2019.12.17.879825 ◽

2019 ◽

Author(s):

T. Barbot ◽

V. Beswick ◽

C. Montigny ◽

E. Quiniou ◽

N. Jamin ◽

...

Keyword(s):

Endoplasmic Reticulum ◽

Conformational Transition ◽

Phosphorylation Site ◽

Normal Modes ◽

General Mechanism ◽

Regulatory Peptide ◽

Mechanism Of Inhibition ◽

Normal Modes Analysis ◽

The Impact

AbstractSERCA1a is an ATPase calcium pump that transports Ca2+ from the cytoplasm to the sarco/endoplasmic reticulum lumen. Sarcolipin (SLN), a transmembrane peptide, regulates the activity of SERCA1a by decreasing its Ca2+ transport rate, but its mechanism of action is still not well understood. To decipher this mechanism, we have performed normal modes analysis in the all-atom model, with the SERCA1a-SLN complex or the isolated SERCA1a embedded in an explicit membrane. The comparison of the results allowed us to provide an explanation for the action of SLN that is in good agreement with experimental observations. In our analyses, the presence of SLN locally perturbs the TM6 transmembrane helix and as a consequence modifies the position of D800, one of the key metal-chelating residues. Additionally, it reduces the flexibility of the gating residues, V304 and E309 in TM4, at the entrance of the Ca2+ binding sites, which would decrease the affinity for Ca2+. Unexpectedly, SLN has also an effect on the ATP binding site more than 35 Å away, due to the straightening of TM5, a long helix considered as the spine of the protein. The straightening of TM5 modifies the structure of the P-N linker that sits above it, and which comprises the 351DKTG354 conserved motif, resulting in an increase of the distance between ATP and the phosphorylation site. As a consequence, the turn-over rate could be affected. All this gives SERCA1a the propensity to go toward a Ca2+-deprived E2-like state in the presence of SLN and toward a Ca2+ high-affinity E1-like state in the absence of SLN, although the SERCA1a-SLN complex was crystallized in an E1-like state. In addition to a general mechanism of inhibition of SERCA1a regulatory peptides, this study also provides an insight in the conformational transition between the E2 and E1 states.Statement of SignificanceThe role of sarco/endoplasmic reticulum calcium ATPase in muscle relaxation is essential. Impairment of its function may result in either cardiac diseases, or myopathies, and also thermogenesis defects. Inhibition of the ATPase by regulatory peptide such as sarcolipin remains unclear. The structure of the ATPase in complex with this peptide was studied by all-atom normal modes analysis, an in silico technique which allows us to decipher the mechanism of inhibition of calcium transport by sarcolipin at a molecular level. Our results open the way to understanding the impact of in vivo misregulation of the ATPase activity by sarcolipin. Development of tools enhancing or preventing interaction between the ATPase and its regulatory peptide could be considered as new therapeutic approaches.

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Protein conformational transitions explored by a morphing approach based on normal mode analysis in internal coordinates

PLoS ONE ◽

10.1371/journal.pone.0258818 ◽

2021 ◽

Vol 16 (11) ◽

pp. e0258818

Author(s):

Byung Ho Lee ◽

Soon Woo Park ◽

Soojin Jo ◽

Moon Ki Kim

Keyword(s):

Normal Mode ◽

Conformational Changes ◽

Degrees Of Freedom ◽

Large Scale ◽

Conformational Transition ◽

Normal Mode Analysis ◽

Mode Analysis ◽

Theoretical Approaches ◽

Internal Coordinates ◽

Transition Pathways

Large-scale conformational changes are essential for proteins to function properly. Given that these transition events rarely occur, however, it is challenging to comprehend their underlying mechanisms through experimental and theoretical approaches. In this study, we propose a new computational methodology called internal coordinate normal mode-guided elastic network interpolation (ICONGENI) to predict conformational transition pathways in proteins. Its basic approach is to sample intermediate conformations by interpolating the interatomic distance between two end-point conformations with the degrees of freedom constrained by the low-frequency dynamics afforded by normal mode analysis in internal coordinates. For validation of ICONGENI, it is applied to proteins that undergo open-closed transitions, and the simulation results (i.e., simulated transition pathways) are compared with those of another technique, to demonstrate that ICONGENI can explore highly reliable pathways in terms of thermal and chemical stability. Furthermore, we generate an ensemble of transition pathways through ICONGENI and investigate the possibility of using this method to reveal the transition mechanisms even when there are unknown metastable states on rough energy landscapes.

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Domain Motions and the Open-to-Closed Conformational Transition of an Enzyme: A Normal Mode Analysis ofS-Adenosyl-l-homocysteine Hydrolase†

Biochemistry ◽

10.1021/bi047524m ◽

2005 ◽

Vol 44 (19) ◽

pp. 7228-7239 ◽

Cited By ~ 16

Author(s):

Mengmeng Wang ◽

Ronald T. Borchardt ◽

Richard L. Schowen ◽

Krzysztof Kuczera

Keyword(s):

Normal Mode ◽

Conformational Transition ◽

Normal Mode Analysis ◽

Mode Analysis ◽

Domain Motions

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Allosteric Conformational Transition in Adenylate Kinase: Dynamic Correlations and Implication for Allostery

Australian Journal of Chemistry ◽

10.1071/ch09449 ◽

2010 ◽

Vol 63 (3) ◽

pp. 405 ◽

Cited By ~ 8

Author(s):

Ming S. Liu ◽

Billy D. Todd ◽

Richard J. Sadus

Keyword(s):

Normal Mode ◽

Conformational Changes ◽

Adenylate Kinase ◽

Conformational Transition ◽

Normal Mode Analysis ◽

Coarse Grained ◽

Mode Analysis ◽

Elastic Network Model ◽

Protein Functions ◽

Correlated Motion

An essential aspect of protein science is to determine the deductive relationship between structure, dynamics, and various sets of functions. The role of dynamics is currently challenging our understanding of protein functions, both experimentally and theoretically. To verify the internal fluctuations and dynamics correlations in an enzyme protein undergoing conformational transitions, we have applied a coarse-grained dynamics algorithm using the elastic network model for adenylate kinase. Normal mode analysis reveals possible dynamical and allosteric pathways for the transition between the open and the closed states of adenylate kinase. As the ligands binding induces significant flexibility changes of the nucleotides monophosphate (NMP) domain and adenosine triphosphate (ATP) domain, the diagonalized correlation between different structural transition states shows that most correlated motions occur between the NMP domain and the helices surrounding the ATP domain. The simultaneous existence of positive and negative correlations indicates that the conformational changes of adenylate kinase take place in an allosteric manner. Analyses of the cumulated normal mode overlap coefficients and long-range correlated motion provide new insights of operating mechanisms and dynamics of adenylate kinase. They also suggest a quantitative dynamics criterion for determining the allosteric cooperativity, which may be applicable to other proteins.

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Application of the ESMACS Binding Free Energy Protocol to a Highly Varied Ligand Dataset: Lactate Dehydogenase A

10.26434/chemrxiv.8398055 ◽

2019 ◽

Author(s):

David Wright ◽

Fouad Husseini ◽

Shunzhou Wan ◽

Christophe Meyer ◽

Herman Van Vlijmen ◽

...

Keyword(s):

Free Energy ◽

Surface Area ◽

Binding Free Energy ◽

Normal Mode Analysis ◽

Binding Mode ◽

Accessible Surface Area ◽

Solvent Accessible Surface Area ◽

Mode Analysis ◽

Energy Calculation ◽

Accessible Surface

<div>Here, we evaluate the performance of our range of ensemble simulation based binding free energy calculation protocols, called ESMACS (enhanced sampling of molecular dynamics with approximation of continuum solvent) for use in fragment based drug design scenarios. ESMACS is designed to generate reproducible binding affinity predictions from the widely used molecular mechanics Poisson-Boltzmann surface area (MMPBSA) approach. We study ligands designed to target two binding pockets in the lactate dehydogenase A target protein, which vary in size, charge and binding mode. When comparing to experimental results, we obtain excellent statistical rankings across this highly diverse set of ligands. In addition, we investigate three approaches to account for entropic contributions not captured by standard MMPBSA calculations: (1) normal mode analysis, (2) weighted solvent accessible surface area (WSAS) and (3) variational entropy. </div>

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RAMAN SPECTRA OF TITANIUM DI-, TRI-, AND TETRA-CHLORIDES

International Journal of Modern Physics B ◽

10.1142/s021797920100886x ◽

2001 ◽

Vol 15 (28n30) ◽

pp. 3865-3868 ◽

Cited By ~ 2

Author(s):

H. MIYAOKA ◽

T. KUZE ◽

H. SANO ◽

H. MORI ◽

G. MIZUTANI ◽

...

Keyword(s):

Force Constant ◽

Raman Spectra ◽

Normal Mode ◽

Raman Band ◽

Normal Mode Analysis ◽

Force Constants ◽

Mode Analysis ◽

Oxidation Number

We have obtained the Raman spectra of TiCl n (n= 2, 3, and 4). Assignments of the observed Raman bands were made by a normal mode analysis. The force constants were determined from the observed Raman band frequencies. We have found that the Ti-Cl stretching force constant increases as the oxidation number of the Ti species increases.

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Normal mode analysis of spectral density of FMO trimers: Intra- and intermonomer energy transfer

The Journal of Chemical Physics ◽

10.1063/5.0027994 ◽

2020 ◽

Vol 153 (21) ◽

pp. 215103

Author(s):

Alexander Klinger ◽

Dominik Lindorfer ◽

Frank Müh ◽

Thomas Renger

Keyword(s):

Energy Transfer ◽

Spectral Density ◽

Normal Mode ◽

Normal Mode Analysis ◽

Mode Analysis

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Normal-mode analysis for scalar fields in BTZ black-hole background

The European Physical Journal C ◽

10.1140/epjc/s10052-009-0870-0 ◽

2009 ◽

Vol 60 (2) ◽

pp. 169-173 ◽

Cited By ~ 6

Author(s):

Sayan K. Chakrabarti ◽

Pulak Ranjan Giri ◽

Kumar S. Gupta

Keyword(s):

Black Hole ◽

Normal Mode ◽

Normal Mode Analysis ◽

Scalar Fields ◽

Mode Analysis ◽

Btz Black Hole ◽

Black Hole Background

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Electrostatic oscillations in cold inhomogeneous plasma I. Differential equation approach

Journal of Plasma Physics ◽

10.1017/s0022377800005754 ◽

1971 ◽

Vol 5 (2) ◽

pp. 239-263 ◽

Cited By ~ 145

Author(s):

Z. Sedláček

Keyword(s):

Differential Equation ◽

Green Function ◽

Normal Mode Analysis ◽

Inhomogeneous Plasma ◽

Mode Analysis ◽

Complex Frequency ◽

Plasma Oscillations ◽

The Laplace Transform ◽

Collective Oscillations ◽

The Green Function

Small amplitude electrostatic oscillations in a cold plasma with continuously varying density have been investigated. The problem is the same as that treated by Barston (1964) but instead of his normal-mode analysis we employ the Laplace transform approach to solve the corresponding initial-value problem. We construct the Green function of the differential equation of the problem to show that there are branch-point singularities on the real axis of the complex frequency-plane, which correspond to the singularities of the Barston eigenmodes and which, asymptotically, give rise to non-collective oscillations with position-dependent frequency and damping proportional to negative powers of time. In addition we find an infinity of new singularities (simple poles) of the analytic continuation of the Green function into the lower half of the complex frequency-plane whose position is independent of the spatial co-ordinate so that they represent collective, exponentially damped modes of plasma oscillations. Thus, although there may be no discrete spectrum, in a more general sense a dispersion relation does exist but must be interpreted in the same way as in the case of Landau damping of hot plasma oscillations.

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Rapid Characterization of Allosteric Networks with Ensemble Normal Mode Analysis

The Journal of Physical Chemistry B ◽

10.1021/acs.jpcb.6b01991 ◽

2016 ◽

Vol 120 (33) ◽

pp. 8276-8288 ◽

Cited By ~ 14

Author(s):

Xin-Qiu Yao ◽

Lars Skjærven ◽

Barry J. Grant

Keyword(s):

Normal Mode ◽

Normal Mode Analysis ◽

Mode Analysis ◽

Rapid Characterization

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