JMS/sandbox9

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Professors Yigal Burstein (Weizmann Institute) and Felix Frolow (Tel Aviv University) studied a<scene name='JMS/sandbox5/Tbadh/1'>thermophilic alcohol dehydrogenase</scene> ([[1ykf]]) from ''T. brockii'' that maintains its structure in over 83℃.
Professors Yigal Burstein (Weizmann Institute) and Felix Frolow (Tel Aviv University) studied a<scene name='JMS/sandbox5/Tbadh/1'>thermophilic alcohol dehydrogenase</scene> ([[1ykf]]) from ''T. brockii'' that maintains its structure in over 83℃.
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They identified two contributing factors to this enzymes thermal prowess. Firstly, he found the thermophilic enzyme had a unique <scene name='JMS/sandbox5/Ion_network/4'>four amino acid binding-network</scene> that encompassed two monomers of the tetrameric enzyme, repeating between each monomer and its two partner monomers. This network apparently makes the oligomer more stable. Secondly, the thermophilic enzyme was <scene name='JMS/sandbox5/Proline/2'>enriched for proline</scene>. Because proline's side chain has minimal degree of freedom, proline's, unlike other amino acids, are minimally restricted by folding. There is therefore a smaller loss of entropy upon folding into the native structure.
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They identified that the hyperthermophilic enzyme was <scene name='JMS/sandbox5/Proline/2'>enriched for proline</scene> in position 275, as was the thermophilic enzyme in position 100. Because proline's side chain has minimal degree of freedom, proline's, unlike other amino acids, are minimally restricted by folding. There is therefore a smaller loss of entropy upon folding into the native structure.
<scene name='JMS/sandbox9/Tbadh/1'>TextToBeDisplayed</scene>
<scene name='JMS/sandbox9/Tbadh/1'>TextToBeDisplayed</scene>

Revision as of 10:31, 14 May 2013

halophilic enzyme (PDB entry 1hlp)

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Joseph M. Steinberger

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