152d: Difference between revisions

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caption="152d, resolution 1.400&Aring;" />
caption="152d, resolution 1.400&Aring;" />
'''DIVERSITY OF WATER RING SIZE AT DNA INTERFACES: HYDRATION AND DYNAMICS OF DNA-ANTHRACYCLINE COMPLEXES'''<br />
'''DIVERSITY OF WATER RING SIZE AT DNA INTERFACES: HYDRATION AND DYNAMICS OF DNA-ANTHRACYCLINE COMPLEXES'''<br />


==Overview==
==Overview==
In crystallographic structures of biological macromolecules, one can, observe many hydration rings that originate at one water molecule, pass, via hydrogen bonds through several others, and return to the original, water molecule. Five-membered water rings have been thought to occur with, greater frequency than other ring sizes. We describe a quantitative, assessment of relationships between water ring size and frequency of, occurrence in the vicinity of nucleic acid interfaces. This report focuses, on low-temperature X-ray crystallographic structures of two, anthracyclines, adriamycin (ADRI) and daunomycin (DAUN), bound to, d(CGATCG) and on several DNA structures published previously by others. We, have obtained excellent low-temperature (-160 degrees C, LT) X-ray, intensity data for d(CGATCG)-adriamycin and d(CGATCG)-daunomycin with a, multiwire area detector. The LTX-ray data sets contain 20% (daunomycin, LT-DAUN) and 35% (adriamycin, LT-ADRI) more reflections than were used to, derive the original room-temperature (15 degrees C) structures [Frederick, C.A., Williams, L.D., Ughetto, G., van der Marel, G. A., van Boom, J.H., Rich, A., &amp; Wang, A.H.-J. (1990) Biochemistry 29, 2538-2549]. The results, show that five-membered water rings are not preferred over other ring, sizes. This assessment is consistent with our observation of broad, dispersion W-W-W angles (sigma = 20 degrees). In addition, we report that, the thermal mobility, distinct from the static disorder, of the amino, sugar of daunomycin and adriamycin is significantly greater than that of, the rest of the complex. This mobility implies that if the central AT base, pair is switched to a CG base pair, there should be a low energy cost in, avoiding the guanine amino group. The energy difference (for the, sugar-binding preference) between d(CGTACG) and d(CGCGCG) could be, considerably less than 20 kcal/mol, a value proposed previously from, computation.
In crystallographic structures of biological macromolecules, one can observe many hydration rings that originate at one water molecule, pass via hydrogen bonds through several others, and return to the original water molecule. Five-membered water rings have been thought to occur with greater frequency than other ring sizes. We describe a quantitative assessment of relationships between water ring size and frequency of occurrence in the vicinity of nucleic acid interfaces. This report focuses on low-temperature X-ray crystallographic structures of two anthracyclines, adriamycin (ADRI) and daunomycin (DAUN), bound to d(CGATCG) and on several DNA structures published previously by others. We have obtained excellent low-temperature (-160 degrees C, LT) X-ray intensity data for d(CGATCG)-adriamycin and d(CGATCG)-daunomycin with a multiwire area detector. The LTX-ray data sets contain 20% (daunomycin, LT-DAUN) and 35% (adriamycin, LT-ADRI) more reflections than were used to derive the original room-temperature (15 degrees C) structures [Frederick, C.A., Williams, L.D., Ughetto, G., van der Marel, G. A., van Boom, J.H., Rich, A., &amp; Wang, A.H.-J. (1990) Biochemistry 29, 2538-2549]. The results show that five-membered water rings are not preferred over other ring sizes. This assessment is consistent with our observation of broad dispersion W-W-W angles (sigma = 20 degrees). In addition, we report that the thermal mobility, distinct from the static disorder, of the amino sugar of daunomycin and adriamycin is significantly greater than that of the rest of the complex. This mobility implies that if the central AT base pair is switched to a CG base pair, there should be a low energy cost in avoiding the guanine amino group. The energy difference (for the sugar-binding preference) between d(CGTACG) and d(CGCGCG) could be considerably less than 20 kcal/mol, a value proposed previously from computation.


==About this Structure==
==About this Structure==
152D is a [http://en.wikipedia.org/wiki/Protein_complex Protein complex] structure of sequences from [http://en.wikipedia.org/wiki/ ] with DM1 as [http://en.wikipedia.org/wiki/ligand ligand]. Full crystallographic information is available from [http://ispc.weizmann.ac.il/oca-bin/ocashort?id=152D OCA].  
152D is a [http://en.wikipedia.org/wiki/Protein_complex Protein complex] structure of sequences from [http://en.wikipedia.org/wiki/ ] with <scene name='pdbligand=DM1:'>DM1</scene> as [http://en.wikipedia.org/wiki/ligand ligand]. Full crystallographic information is available from [http://oca.weizmann.ac.il/oca-bin/ocashort?id=152D OCA].  


==Reference==
==Reference==
Water ring structure at DNA interfaces: hydration and dynamics of DNA-anthracycline complexes., Lipscomb LA, Peek ME, Zhou FX, Bertrand JA, VanDerveer D, Williams LD, Biochemistry. 1994 Mar 29;33(12):3649-59. PMID:[http://ispc.weizmann.ac.il//pmbin/getpm?pmid=8142363 8142363]
Water ring structure at DNA interfaces: hydration and dynamics of DNA-anthracycline complexes., Lipscomb LA, Peek ME, Zhou FX, Bertrand JA, VanDerveer D, Williams LD, Biochemistry. 1994 Mar 29;33(12):3649-59. PMID:[http://ispc.weizmann.ac.il//pmbin/getpm?pmid=8142363 8142363]
[[Category: Protein complex]]
[[Category: Protein complex]]
[[Category: Bertrand, J.A.]]
[[Category: Bertrand, J A.]]
[[Category: Lipscomb, L.A.]]
[[Category: Lipscomb, L A.]]
[[Category: Peek, M.E.]]
[[Category: Peek, M E.]]
[[Category: VanDerveer, D.]]
[[Category: VanDerveer, D.]]
[[Category: Williams, L.D.]]
[[Category: Williams, L D.]]
[[Category: Zhou, F.X.]]
[[Category: Zhou, F X.]]
[[Category: DM1]]
[[Category: DM1]]
[[Category: complexed with drug]]
[[Category: complexed with drug]]
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[[Category: right handed dna]]
[[Category: right handed dna]]


''Page seeded by [http://ispc.weizmann.ac.il/oca OCA ] on Sat Nov 24 21:58:22 2007''
''Page seeded by [http://oca.weizmann.ac.il/oca OCA ] on Thu Feb 21 11:38:21 2008''

Revision as of 12:38, 21 February 2008

File:152d.gif


152d, resolution 1.400Å

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DIVERSITY OF WATER RING SIZE AT DNA INTERFACES: HYDRATION AND DYNAMICS OF DNA-ANTHRACYCLINE COMPLEXES

OverviewOverview

In crystallographic structures of biological macromolecules, one can observe many hydration rings that originate at one water molecule, pass via hydrogen bonds through several others, and return to the original water molecule. Five-membered water rings have been thought to occur with greater frequency than other ring sizes. We describe a quantitative assessment of relationships between water ring size and frequency of occurrence in the vicinity of nucleic acid interfaces. This report focuses on low-temperature X-ray crystallographic structures of two anthracyclines, adriamycin (ADRI) and daunomycin (DAUN), bound to d(CGATCG) and on several DNA structures published previously by others. We have obtained excellent low-temperature (-160 degrees C, LT) X-ray intensity data for d(CGATCG)-adriamycin and d(CGATCG)-daunomycin with a multiwire area detector. The LTX-ray data sets contain 20% (daunomycin, LT-DAUN) and 35% (adriamycin, LT-ADRI) more reflections than were used to derive the original room-temperature (15 degrees C) structures [Frederick, C.A., Williams, L.D., Ughetto, G., van der Marel, G. A., van Boom, J.H., Rich, A., & Wang, A.H.-J. (1990) Biochemistry 29, 2538-2549]. The results show that five-membered water rings are not preferred over other ring sizes. This assessment is consistent with our observation of broad dispersion W-W-W angles (sigma = 20 degrees). In addition, we report that the thermal mobility, distinct from the static disorder, of the amino sugar of daunomycin and adriamycin is significantly greater than that of the rest of the complex. This mobility implies that if the central AT base pair is switched to a CG base pair, there should be a low energy cost in avoiding the guanine amino group. The energy difference (for the sugar-binding preference) between d(CGTACG) and d(CGCGCG) could be considerably less than 20 kcal/mol, a value proposed previously from computation.

About this StructureAbout this Structure

152D is a Protein complex structure of sequences from [1] with as ligand. Full crystallographic information is available from OCA.

ReferenceReference

Water ring structure at DNA interfaces: hydration and dynamics of DNA-anthracycline complexes., Lipscomb LA, Peek ME, Zhou FX, Bertrand JA, VanDerveer D, Williams LD, Biochemistry. 1994 Mar 29;33(12):3649-59. PMID:8142363

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