Journal:JBSD:24
From Proteopedia
(Difference between revisions)
| Line 4: | Line 4: | ||
<hr/> | <hr/> | ||
<b>Molecular Tour</b><br> | <b>Molecular Tour</b><br> | ||
| + | Drug resistance has been an urgent problem that severely limits the therapy of current clinical microbial diseases. Sometimes, it generally correlates with mutations to the dihydropteroate synthase (DHPS) gene. | ||
| + | In the current study, we focus on the molecular dynamic behaviors and binding free energy calculations of wild-type (wt) form and mutated form B. anthracis dihydropteroate synthase (BaDHPS) to search for the relationship between mutation and drug resistance. | ||
| + | After 20ns MD simulations on the wt form and mutated form enzymes, it is obvious that mutation D184N and K220Q have much lower binding affinity to the inhibitor DHP-STZ than the wt form enzyme. Mutation will cause conformational change, which mainly locate on some loop region around the binding site (Loop 1, Loop 2 and Loop 7). These results may be helpful for further drug resistance and de novo drug design investigations. | ||
</StructureSection> | </StructureSection> | ||
Revision as of 08:15, 2 September 2012
| |||||||||||
- ↑ REF
This page complements a publication in scientific journals and is one of the Proteopedia's Interactive 3D Complement pages. For aditional details please see I3DC.
