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User:Karsten Theis/overall views

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< User:Karsten Theis(Difference between revisions)
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__NOTOC__
==Introduction==
==Introduction==
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This is a collection of how protein structures are depicted in publications. The most common views show
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<gallery>
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* domains
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Image:UvrB fold.JPG
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* conservation
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Image:UvrB charge.JPG
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Image:UvrB slab core.JPG
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Image:UvrB consurf.JPG
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</gallery>
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This is a collection of how entire protein structures are depicted in publications. The most common views show
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* fold of domains
* charge distribution
* charge distribution
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* contact interfaces
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* hydrophobic patches
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* surface conservation
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* superpositions with related structures
==Standard and other views==
==Standard and other views==
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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.
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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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==Types of overall views==
==Types of overall views==
<StructureSection load='1d9z' size='340' side='right' caption='Automatically generated figure for UvrB structure, PDBID 1d9z' scene=''>
<StructureSection load='1d9z' size='340' side='right' caption='Automatically generated figure for UvrB structure, PDBID 1d9z' scene=''>
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===Ribbon diagram showing secondary structure===
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===Ribbon diagram showing fold===
[[Image:UvrB fold.JPG|none|thumb|200px]]
[[Image:UvrB fold.JPG|none|thumb|200px]]
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The first view of a protein shown in a publication is often a cartoon of the <scene name='78/780454/Domains/7'>secondary structure colored by domains</scene>.
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The first view of a protein shown in a publication is often a cartoon of the <scene name='78/780454/Domains/7'>fold colored by domains</scene>. The fold of a protein refers to how secondary structure elements are assembled in three dimensions, and it is often shown in a cartoon (Richardson diagram).
<jmol>
<jmol>
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<script>
<script>
select protein; define ~consurf_to_do selected
select protein; define ~consurf_to_do selected
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consurf_initial_scene = true; script "/wiki/ConSurf/d9/1d9z_consurf.spt"
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consurf_initial_scene = true; script "/wiki/ConSurf/d9/1d9z_consurf.spt";select protein;spacefill only
</script>
</script>
<text>conservation</text>
<text>conservation</text>
</jmolLink>
</jmolLink>
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</jmol>, we use data from [[Introduction to Evolutionary Conservation|ConSurf]].
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</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).
<jmol>
<jmol>
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<jmol>
<jmol>
<jmolCheckbox>
<jmolCheckbox>
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<scriptWhenChecked>select 415-600;rotateselected {558.CA}{580.CA} 120 -0.5</scriptWhenChecked>
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<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>
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This superposition is complicated. Try hiding some of the elements to see clearer, and open a popup 3D browser to view a larger version. Also, rotate the molecules a bit to see them from different angles. You can use the wobble button at the bottom of the page as well. In the original publication [http://emboj.embopress.org/content/18/24/6899.figures-only](Fig. 4), the figure is shown in stereo for better viewing, and domain 2 is omitted. Here, you can turn on stereo as well. The is best done in the pop-up window using the right-click menu, but depending on your eyes, you might need stereo glasses to experience the effect.
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This superposition is complicated. Try hiding some of the elements to see clearer, and open a popup 3D browser to view a larger version. Also, rotate the molecules a bit to see them from different angles. You can use the wobble button at the bottom of the page as well. In the original publication [http://emboj.embopress.org/content/18/24/6899.figures-only](Fig. 4), the figure is shown in stereo for better viewing, and domain 2 is omitted. In the Jmol browser used here, you can turn on stereo as well. This is best done in the pop-up window using the right-click menu, but depending on your eyes, you might need stereo glasses to experience the effect.
<jmol>
<jmol>

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

Automatically generated figure for UvrB structure, PDBID 1d9z

Drag the structure with the mouse to rotate

References

  1. 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

Proteopedia Page Contributors and Editors (what is this?)

Karsten Theis

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