Abstract
<div class="line" id="line-13"> <span style='color: rgb(28, 29, 30); font-family: "Open Sans", icomoon, sans-serif; font-size: 16px;'> This short article examines the usefulness of fast simulations of conformational transition paths in elucidating enzymatic mechanisms and guiding drug discovery for protein kinases. It applies the transition path method in the MOIL software package to simulate the paths of conformational transitions between six pairs of structures from the Protein Data Bank. The structures along the transition paths were found to resemble experimental structures that mimic transient structures believed to form during enzymatic catalysis or conformational transitions, or structures that have drug candidates bound. These findings suggest that such simulations could provide quick initial insights into the enzymatic mechanisms or pathways of conformational transitions of proteins kinases, or could provide structures useful for aiding structure‐based drug design. </span></div>
Original language | American English |
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Journal | Protein Science |
Volume | 25 |
DOIs | |
State | Published - Jan 1 2016 |
Keywords
- catalytic mechanisms of protein kinases
- conformational transition paths
- protein kinases
- structures for ensemble docking
Disciplines
- Biochemistry