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==Overview==
==Overview==
Crystal structures of catalytic domains of MMP-3 and MT1-MMP bound to, TIMP-1 or TIMP-2, respectively, differ in the orientation of the TIMP in, the MMP active site. The orientation in solution of N-TIMP-1 in the MMP-3, active site has been investigated using residual dipolar couplings (RDCs)., Fitting of the RDCs to the X-ray structures of the complexes suggests, general agreement with the orientation of crystalline MMP-3(DeltaC) and, TIMP-1 and a large disparity from the orientation of crystalline, MT1-MMP(DeltaC) and TIMP-2. Rigid body docking of MMP-3 and N-TIMP-1 X-ray, coordinates using RDCs and intermolecular NOEs provided a time-averaged, orientation in solution differing from the crystal structure by a 5, degrees rotation toward the MT1-MMP(DeltaC)/TIMP-2 orientation. The slight, discrepancy in orientations in solution and crystal lies within the, experimental uncertainties. Intermolecular NOEs used in the docking, corroborated the accuracy of mapping the interface by a paramagnetic NMR, footprinting assay, a potential alternative source of contacts for, docking. Some uncertainty in the N-TIMP-1 orientation in the MMP-3 active, site, coupled with microsecond to millisecond fluctuations of the, MMP-binding ridge of N-TIMP-1 in the complex and flexibility in, MMP-3(DeltaC) S(1)' to S(3)' subsites, leaves open the possibility that, N-TIMP-1 might dynamically pivot a few degrees or more in the arc toward, the MT1-MMP(DeltaC)/TIMP-2 orientation. Differing TIMP orientations in MMP, active sites are more likely to result from structural differences in TIMP, AB hairpin loops than from crystal packing artifacts.
Crystal structures of catalytic domains of MMP-3 and MT1-MMP bound to TIMP-1 or TIMP-2, respectively, differ in the orientation of the TIMP in the MMP active site. The orientation in solution of N-TIMP-1 in the MMP-3 active site has been investigated using residual dipolar couplings (RDCs). Fitting of the RDCs to the X-ray structures of the complexes suggests general agreement with the orientation of crystalline MMP-3(DeltaC) and TIMP-1 and a large disparity from the orientation of crystalline MT1-MMP(DeltaC) and TIMP-2. Rigid body docking of MMP-3 and N-TIMP-1 X-ray coordinates using RDCs and intermolecular NOEs provided a time-averaged orientation in solution differing from the crystal structure by a 5 degrees rotation toward the MT1-MMP(DeltaC)/TIMP-2 orientation. The slight discrepancy in orientations in solution and crystal lies within the experimental uncertainties. Intermolecular NOEs used in the docking corroborated the accuracy of mapping the interface by a paramagnetic NMR footprinting assay, a potential alternative source of contacts for docking. Some uncertainty in the N-TIMP-1 orientation in the MMP-3 active site, coupled with microsecond to millisecond fluctuations of the MMP-binding ridge of N-TIMP-1 in the complex and flexibility in MMP-3(DeltaC) S(1)' to S(3)' subsites, leaves open the possibility that N-TIMP-1 might dynamically pivot a few degrees or more in the arc toward the MT1-MMP(DeltaC)/TIMP-2 orientation. Differing TIMP orientations in MMP active sites are more likely to result from structural differences in TIMP AB hairpin loops than from crystal packing artifacts.


==Disease==
==Disease==
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[[Category: Stromelysin 1]]
[[Category: Stromelysin 1]]
[[Category: Arumugam, S.]]
[[Category: Arumugam, S.]]
[[Category: Doren, S.R.Van.]]
[[Category: Doren, S R.Van.]]
[[Category: protein-protein complex]]
[[Category: protein-protein complex]]


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Revision as of 15:19, 21 February 2008

File:1oo9.jpg


1oo9

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Orientation in Solution of MMP-3 Catalytic Domain and N-TIMP-1 from Residual Dipolar Couplings

OverviewOverview

Crystal structures of catalytic domains of MMP-3 and MT1-MMP bound to TIMP-1 or TIMP-2, respectively, differ in the orientation of the TIMP in the MMP active site. The orientation in solution of N-TIMP-1 in the MMP-3 active site has been investigated using residual dipolar couplings (RDCs). Fitting of the RDCs to the X-ray structures of the complexes suggests general agreement with the orientation of crystalline MMP-3(DeltaC) and TIMP-1 and a large disparity from the orientation of crystalline MT1-MMP(DeltaC) and TIMP-2. Rigid body docking of MMP-3 and N-TIMP-1 X-ray coordinates using RDCs and intermolecular NOEs provided a time-averaged orientation in solution differing from the crystal structure by a 5 degrees rotation toward the MT1-MMP(DeltaC)/TIMP-2 orientation. The slight discrepancy in orientations in solution and crystal lies within the experimental uncertainties. Intermolecular NOEs used in the docking corroborated the accuracy of mapping the interface by a paramagnetic NMR footprinting assay, a potential alternative source of contacts for docking. Some uncertainty in the N-TIMP-1 orientation in the MMP-3 active site, coupled with microsecond to millisecond fluctuations of the MMP-binding ridge of N-TIMP-1 in the complex and flexibility in MMP-3(DeltaC) S(1)' to S(3)' subsites, leaves open the possibility that N-TIMP-1 might dynamically pivot a few degrees or more in the arc toward the MT1-MMP(DeltaC)/TIMP-2 orientation. Differing TIMP orientations in MMP active sites are more likely to result from structural differences in TIMP AB hairpin loops than from crystal packing artifacts.

DiseaseDisease

Known diseases associated with this structure: Coronary heart disease, susceptibility to OMIM:[185250], Sorsby fundus dystrophy OMIM:[188826]

About this StructureAbout this Structure

1OO9 is a Protein complex structure of sequences from Homo sapiens. Active as Stromelysin 1, with EC number 3.4.24.17 Full crystallographic information is available from OCA.

ReferenceReference

Global orientation of bound MMP-3 and N-TIMP-1 in solution via residual dipolar couplings., Arumugam S, Van Doren SR, Biochemistry. 2003 Jul 8;42(26):7950-8. PMID:12834347

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