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User:Karsten Theis/overall views
From Proteopedia
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==Standard and other views== | ==Standard and other views== | ||
| - | In publications where figures are two dimensional and non-interactive, researchers have to choose a view that shows as much of the interesting features of the protein as possible. Often, when that is not possible, there will be two orthoganal views (e.g. the second rotated by 90 or 180 degrees. The protein used as an example here is the DNA repair enzyme UvrB in complex with ATP (PDB ID 1d9z). This protein not only binds to ATP, but also to DNA and to another DNA repair protein, UvrA. As you look at the various ways protein structures are depicted, you can zoom in to the different binding surfaces or zoom out to the standard view showing the entire protein with the "business" side facing you. | + | In publications where figures are two dimensional and non-interactive, researchers have to choose a view that shows as much of the interesting features of the protein as possible. Often, when that is not possible, there will be two orthoganal views (e.g. the second rotated by 90 or 180 degrees. The protein used as an example here is the DNA repair enzyme UvrB in complex with ATP (PDB ID 1d9z)<ref>PMID:10601012</ref>. This protein not only binds to ATP, but also to DNA and to another DNA repair protein, UvrA. As you look at the various ways protein structures are depicted, you can zoom in to the different binding surfaces or zoom out to the standard view showing the entire protein with the "business" side facing you. |
<jmol> | <jmol> | ||
<jmolButton> | <jmolButton> | ||
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</jmolButton> | </jmolButton> | ||
</jmol> | </jmol> | ||
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<jmol> | <jmol> | ||
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</jmolButton> | </jmolButton> | ||
</jmol> | </jmol> | ||
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<jmol> | <jmol> | ||
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<text>conservation</text> | <text>conservation</text> | ||
</jmolLink> | </jmolLink> | ||
| - | </jmol>, we use data from [[Introduction to Evolutionary Conservation|ConSurf]]. | + | </jmol>, we use data from [[Introduction to Evolutionary Conservation|ConSurf]] (scene <scene name='78/780454/Conservation/1'>oriented as 2D figure</scene> on the left). |
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<jmol> | <jmol> | ||
<jmolCheckbox> | <jmolCheckbox> | ||
| - | <scriptWhenChecked>select 415-600;rotateselected {558.CA}{580.CA} 120 | + | <scriptWhenChecked>select 415-600;rotateselected {558.CA}{580.CA} 120 </scriptWhenChecked> |
<scriptWhenUnchecked>select 415-600;rotateselected {558.CA}{580.CA} -120</scriptWhenUnchecked> | <scriptWhenUnchecked>select 415-600;rotateselected {558.CA}{580.CA} -120</scriptWhenUnchecked> | ||
<checked>false</checked> | <checked>false</checked> | ||
Current revision
Introduction
This is a collection of how entire protein structures are depicted in publications. The most common views show
- fold of domains
- charge distribution
- hydrophobic patches
- surface conservation
- superpositions with related structures
Standard and other views
In publications where figures are two dimensional and non-interactive, researchers have to choose a view that shows as much of the interesting features of the protein as possible. Often, when that is not possible, there will be two orthoganal views (e.g. the second rotated by 90 or 180 degrees. The protein used as an example here is the DNA repair enzyme UvrB in complex with ATP (PDB ID 1d9z)[1]. This protein not only binds to ATP, but also to DNA and to another DNA repair protein, UvrA. As you look at the various ways protein structures are depicted, you can zoom in to the different binding surfaces or zoom out to the standard view showing the entire protein with the "business" side facing you.
Types of overall views
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References
- ↑ Theis K, Chen PJ, Skorvaga M, Van Houten B, Kisker C. Crystal structure of UvrB, a DNA helicase adapted for nucleotide excision repair. EMBO J. 1999 Dec 15;18(24):6899-907. PMID:10601012 doi:10.1093/emboj/18.24.6899
