Open AccessForce Field Effects in Simulations of Flexible Peptides with Varying Polyproline II Propensity
Author(s) -
Stéphanie Jephthah,
Francesco Pesce,
Kresten LindorffLarsen,
Marie Skepö
Publication year - 2021
Publication title -
journal of chemical theory and computation
Language(s) - English
Resource type - Journals
SCImago Journal Rank - 2.001
H-Index - 185
eISSN - 1549-9626
pISSN - 1549-9618
DOI - 10.1021/acs.jctc.1c00408
Subject(s) - polyproline helix , force field (fiction) , molecular dynamics , protein secondary structure , chemical physics , chemistry , circular dichroism , biological system , computational chemistry , crystallography , peptide , physics , nuclear magnetic resonance , biology , quantum mechanics
Five peptides previously suggested to possess polyproline II (PPII) structure have here been investigated by using atomistic molecular dynamics simulations to compare how well four different force fields known for simulating intrinsically disordered proteins relatively well (Amber ff99SB-disp, Amber ff99SB-ILDN, CHARM36IDPSFF, and CHARMM36m) can capture this secondary structure element. The results revealed that all force fields sample PPII structures but to different extents and with different propensities toward other secondary structure elements, in particular, the β-sheet and "random coils". A cluster analysis of the simulations of histatin 5 also revealed that the conformational ensembles of the force fields are quite different. We compared the simulations to circular dichroism and nuclear magnetic resonance spectroscopy experiments and conclude that further experiments and methods for interpreting them are needed to assess the accuracy of force fields in determining PPII structure.