Datasets and analyses of molecular dynamics simulations of covalent binary and ternary complexes of MHC class I-related molecule/T-cell receptor (MR1/TCR) agonists to understand complex formation and conditions of fluorescent labelling

Anke Steinmetz; Thomas Yvorra; Pascal Retailleau; Olivier Lantz; Frédéric Schmidt

Data in Brief (Feb 2021)

Datasets and analyses of molecular dynamics simulations of covalent binary and ternary complexes of MHC class I-related molecule/T-cell receptor (MR1/TCR) agonists to understand complex formation and conditions of fluorescent labelling

Anke Steinmetz,
Thomas Yvorra,
Pascal Retailleau,
Olivier Lantz,
Frédéric Schmidt

Affiliations

Anke Steinmetz: Centre de Recherche et Développement Vitry-Alfortville, IDD/ISDD, Sanofi-Aventis R&D, Vitry-surSeine, 94400, France; Corresponding authors.
Thomas Yvorra: Institut Curie, PSL University, CNRS UMR3666, INSERM U1143, Paris, 75005, France
Pascal Retailleau: Institut de Chimie des Substances Naturelles, CNRS UPR 2301, Université Paris-Saclay, 1 avenue de la Terrasse, Gif-sur-Yvette, 91190, France
Olivier Lantz: Institut Curie, PSL University, INSERM U932, Paris, 75005, France; Institut Curie; Laboratoire d'Immunologie Clinique, Paris, 75005, France; Centre d'Investigation Clinique en Biothérapie, Institut Curie (CIC-BT1428), Paris, 75005, France
Frédéric Schmidt: Institut Curie, PSL University, CNRS UMR3666, INSERM U1143, Paris, 75005, France; Corresponding authors.

Journal volume & issue: Vol. 34
p. 106704

Abstract

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Data of molecular dynamics (MD) simulations were obtained for mucosal-associated invariant T (MAIT) cell ligands complexed with MR1 or MR1/TCR. Ligands included in the simulations were natural ligands 5-(2-oxoethylideneamino)-6-D-ribitylaminouracil (5-OE-RU), 5-(2-oxopropylideneamino)-6-(D-ribitylamino)uracil (5-OP-RU), their C5’ ethinylated analogs in S or R configuration, as well as the corresponding fluorophore-reacted products. All-atom models of the binary and ternary complexes were constructed using PDB entry 4NQE and docked poses [1]. Missing loops, N- and C-termini were completed by homology modelling, the loop conformations optimized, and the models energy minimized prior to setup for MD simulations. A standard pre-equilibration protocol was applied before the production phase of 120 ns simulation as NPT ensemble at 300 K and 1 atm applying an explicit solvent model with OPLS3 force field parameters. Atomic coordinates and energies were recorded every 60 ps and 12 ps, respectively. The corresponding raw data files of the MD simulations are part of this dataset. All simulations were analysed with respect to root mean square deviations (rmsd) and root mean square fluctuations (rmsf) of the coordinates of protein and ligand atoms, stability of protein secondary structure, protein-ligand contacts, ligand torsion profiles, and ligand properties. More detailed statistics of non-covalent interaction counts were also collected. Radial distribution functions (rdf) were calculated when relevant. Visualization of the trajectories permits appreciation of the molecular dynamics of both, ligands and proteins and their interactions, thereby supporting drug design of MAIT cell ligands; furthermore, additional analysis of e.g. conformational changes or interactions not reported in the primary publication [1] can be performed on the data. The raw data may also be used as starting point for extension of the simulations or more sophisticated MD techniques.

Published in Data in Brief

ISSN: 2352-3409 (Online)
Publisher: Elsevier
Country of publisher: United States
LCC subjects: Medicine: Medicine (General): Computer applications to medicine. Medical informatics; Science: Science (General)
Website: http://www.journals.elsevier.com/data-in-brief/

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