Journal:Proteins:2

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Two mutations, <scene name='73/733982/Cv5/9'>T92I, and P211T</scene> (in darkmagenta), are assigned low impact by both computational methods. Both sets of experimental results show close to normal activity and protein levels, consistent with the analysis results. Also reasonably consistent, T92I is assigned to the mild MHP category of disease, suggesting a subtle effect on protein function. Inconsistent with both experiment and computational analysis, P211T is assigned to the “classic PKU” category, based on a single functionally hemizygous patient genotype.
Two mutations, <scene name='73/733982/Cv5/9'>T92I, and P211T</scene> (in darkmagenta), are assigned low impact by both computational methods. Both sets of experimental results show close to normal activity and protein levels, consistent with the analysis results. Also reasonably consistent, T92I is assigned to the mild MHP category of disease, suggesting a subtle effect on protein function. Inconsistent with both experiment and computational analysis, P211T is assigned to the “classic PKU” category, based on a single functionally hemizygous patient genotype.
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'''Evolutionary conservation'''
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<scene name='73/733982/Cv4/36'>Evolutionary conservation</scene>
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{{Template:ColorKey_ConSurf}}
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{{Template:ColorKey_ConSurf_NoYellow}}
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{{Template:ColorKey_ConSurf_NoGray}}
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{{Template:ColorKey_ConSurf_NoYellow_NoGray}}
</StructureSection>
</StructureSection>

Revision as of 11:08, 10 July 2016

PDB ID 2pah

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  1. Shi Z, Sellers J, Moult J. Protein stability and in vivo concentration of missense mutations in phenylalanine hydroxylase. Proteins. 2012 Jan;80(1):61-70. doi: 10.1002/prot.23159. Epub 2011 Sep 21. PMID:21953985 doi:http://dx.doi.org/10.1002/prot.23159

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