Journal:JBSD:24

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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.
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 <scene name='Journal:JBSD:24/Cv/2'>wild-type (wt)</scene> form and <scene name='Journal:JBSD:24/Cv/3'>mutated forms</scene> ''B. anthracis'' dihydropteroate synthase (BaDHPS) to search for the relationship between mutation and drug resistance. <font color='darkmagenta'><b>Wt-BaDHPS is colored in darkmagenta</b></font>, mutated <span style="color:lime;background-color:black;font-weight:bold;">D184N complex is in green</span> and <span style="color:cyan;background-color:black;font-weight:bold;">K220Q complex is in cyan</span>.
In the current study, we focus on the molecular dynamic behaviors and binding free energy calculations of <scene name='Journal:JBSD:24/Cv/2'>wild-type (wt)</scene> form and <scene name='Journal:JBSD:24/Cv/3'>mutated forms</scene> ''B. anthracis'' dihydropteroate synthase (BaDHPS) to search for the relationship between mutation and drug resistance. <font color='darkmagenta'><b>Wt-BaDHPS is colored in darkmagenta</b></font>, mutated <span style="color:lime;background-color:black;font-weight:bold;">D184N complex is in green</span> and <span style="color:cyan;background-color:black;font-weight:bold;">K220Q complex is in cyan</span>.
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After 20ns MD simulations on the <scene name='Journal:JBSD:24/Cv/5'>wt form and mutated form enzymes</scene>, it is obvious that <scene name='Journal:JBSD:24/Cv/8'>mutation D184N and K220Q have much lower binding affinity to the inhibitor DHP-STZ than the wt form enzyme</scene>. Ligand DHP-STZ is colored in the same color as the corresponding protein: for <font color='darkmagenta'><b>Wt-BaDHPS is in darkmagenta</b></font>, for mutated <span style="color:lime;background-color:black;font-weight:bold;">D184N complex is in green</span> and for <span style="color:cyan;background-color:black;font-weight:bold;">K220Q complex is in cyan</span>. 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.
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After 20ns MD simulations on the <scene name='Journal:JBSD:24/Cv/5'>wt form and mutated form enzymes</scene>, it is obvious that <scene name='Journal:JBSD:24/Cv/8'>mutation D184N and K220Q have much lower binding affinity to the inhibitor DHP-STZ than the wt form enzyme</scene>. Only Loop 1, Loop 2 and Loop 7 are colored, ligand DHP-STZ is colored in the same color as the corresponding protein: for <font color='darkmagenta'><b>Wt-BaDHPS is in darkmagenta</b></font>, for mutated <span style="color:lime;background-color:black;font-weight:bold;">D184N complex is in green</span> and for <span style="color:cyan;background-color:black;font-weight:bold;">K220Q complex is in cyan</span>. 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 06:49, 5 September 2012

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