Journal
JOURNAL OF PHYSICAL CHEMISTRY LETTERS
Volume 5, Issue 21, Pages 3614-3619Publisher
AMER CHEMICAL SOC
DOI: 10.1021/jz5018703
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Funding
- EPSRC [EP/F032773/1, EP/J017639/1, EP/F038038/1, EP/G007705/01]
- CCPBioSim project [EP/J010588/1]
- EPSRC [EP/G007705/1, EP/J010588/1, EP/F038038/1, EP/J017639/1, EP/J015059/1, EP/F032773/1] Funding Source: UKRI
- Engineering and Physical Sciences Research Council [EP/J015059/1, EP/F038038/1, EP/F032773/1, EP/J017639/1, EP/J010588/1, EP/G007705/1] Funding Source: researchfish
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Linear-scaling quantum mechanical density functional theory calculations have been applied to study the rearrangement of chorismate to prephenate in large-scale models of the Bacillus subtilis chorismate mutase enzyme. By treating up to 2000 atoms at a consistent quantum mechanical level of theory, we obtain an unbiased, almost parameter-free description of the transition state geometry and energetics. The activation energy barrier is calculated to be lowered by 10.5 kcal mol(-1) in the enzyme, compared with the equivalent reaction in water, which is in good agreement with experiment. Natural bond orbital analysis identifies a number of active site residues that are important for transition state stabilization in chorismate mutase. This benchmark study demonstrates that linear-scaling density functional theory techniques are capable of simulating entire enzymes at the ab initio quantum mechanical level of accuracy. [GRAPHICS]
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