Low-mass molecular dynamics simulation: A simple and generic technique to enhance configurational sampling |
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Authors: | Yuan-Ping Pang |
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Institution: | Computer-Aided Molecular Design Laboratory, Mayo Clinic, Rochester, MN 55905, USA |
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Abstract: | CLN025 is one of the smallest fast-folding proteins. Until now it has not been reported that CLN025 can autonomously fold to its native conformation in a classical, all-atom, and isothermal–isobaric molecular dynamics (MD) simulation. This article reports the autonomous and repeated folding of CLN025 from a fully extended backbone conformation to its native conformation in explicit solvent in multiple 500-ns MD simulations at 277 K and 1 atm with the first folding event occurring as early as 66.1 ns. These simulations were accomplished by using AMBER forcefield derivatives with atomic masses reduced by 10-fold on Apple Mac Pros. By contrast, no folding event was observed when the simulations were repeated using the original AMBER forcefields of FF12SB and FF14SB. The results demonstrate that low-mass MD simulation is a simple and generic technique to enhance configurational sampling. This technique may propel autonomous folding of a wide range of miniature proteins in classical, all-atom, and isothermal–isobaric MD simulations performed on commodity computers—an important step forward in quantitative biology. |
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Keywords: | MD molecular dynamics LMD low-mass molecular dynamics NMR nuclear magnetic resonance CαβRMSD Cα and Cβ root mean square deviation CRMSD all carbon atom root mean square deviation |
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