Residual dipolar coupling derived orientational constraints on ligand geometry in a 53 kDa protein-ligand complex.
The geometric relationships between ligands and the functional groups that bind ligands in soluble ligand-protein complexes have traditionally been deduced from distance constraints between pairs of NMR active nuclei spanning the ligand-protein interface. Frequently, the steep inverse distance dependence of the nuclear Overhauser effect (NOE), from which the distance constraints are derived, makes identification of sufficient numbers of constraints difficult. In these cases the ability to supplement NOE-derived information with distance-independent angular information can be very important. Here, the observation of residual dipolar couplings from alpha-methyl mannose bound to mannose binding-protein in a dilute liquid crystalline medium has allowed the determination of a bound ligand's average orientation. The 3-fold rotational symmetry of mannose-binding protein defines its orientational tensor and obviates the need to determine experimentally the protein's average orientation. Through superimposition of ligand and protein orientational tensors we describe the binding geometry of alpha-methyl mannose bound to mannose-binding protein. This new method is of general applicability to the study of ligands bound to proteins, and it is of particular interest when neither X-ray crystallography nor NOE techniques can provide sufficient information to describe binding geometries.
Duke Scholars
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- Protein Structure, Secondary
- Protein Conformation
- Protein Binding
- Models, Molecular
- Methylmannosides
- Magnetic Resonance Spectroscopy
- Collectins
- Carrier Proteins
- Biochemistry & Molecular Biology
- Binding Sites
Citation
Published In
DOI
ISSN
Publication Date
Volume
Issue
Start / End Page
Location
Related Subject Headings
- Protein Structure, Secondary
- Protein Conformation
- Protein Binding
- Models, Molecular
- Methylmannosides
- Magnetic Resonance Spectroscopy
- Collectins
- Carrier Proteins
- Biochemistry & Molecular Biology
- Binding Sites