Exploring the most stable aptamer/target molecule complex by the stochastic tunnelling-basin hopping-discrete molecular dynamics method
CH Su and HL Chen and SP Ju and TD You and YS Lin and TF Tseng, SCIENTIFIC REPORTS, 11, 11406 (2021).
DOI: 10.1038/s41598-021-90907-y
The stochastic tunnelling-basin hopping-discrete molecular dynamics (STUN-BH-DMD) method was applied to the search for the most stable biomolecular complexes in water by using the MARTINI coarse-grained (CG) model. The epithelial cell adhesion molecule (EpCAM, PDB code: 4MZV) was used as an EpCAM adaptor for an EpA (Apt(EpA)) benchmark target molecule. The effects of two adsorption positions on the EpCAM were analysed, and it is found that the Apt(EpA) adsorption configuration located within the EpCAM pocket-like structure is more stable and the energy barrier is lower due to the interaction with water. By the root mean square deviation (RMSD), the configuration of EpCAM in water is more conservative when the Apt(EpA) binds to EpCAM by attaching to the pocket space of the EpCAM dimer. For Apt(EpA), the root mean square fluctuation (RMSF) analysis result indicates Nucleobase 1 and Nucleobase 2 display higher flexibility during the CGMD simulation. Finally, from the binding energy contour maps and histogram plots of EpCAM and each Apt(EpA) nucleobase, it is clear that the binding energy adsorbed to the pocket-like structure is more continuous than that energy not adsorbed to the pocket-like structure. This study has proposed a new numerical process for applying the STUN-BH-DMD with the CG model, which can reduce computational details and directly find a more stable Apt(EpA)/EpCAM complex in water.
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