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PDBsum entry 1fsb
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Cell adhesion protein
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PDB id
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1fsb
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References listed in PDB file
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Key reference
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Title
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Structure and function of the epidermal growth factor domain of p-Selectin.
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Authors
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S.J.Freedman,
D.G.Sanford,
W.W.Bachovchin,
B.C.Furie,
J.D.Baleja,
B.Furie.
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Ref.
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Biochemistry, 1996,
35,
13733-13744.
[DOI no: ]
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PubMed id
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Abstract
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P-selectin is a multidomain adhesion protein on the surface of activated
platelets and endothelial cells that functions in the recruitment of leukocytes
to the site of inflammation. The amino-terminal lectin and EGF domains
constitute the ligand recognition unit. We have produced a synthetic 40-residue
P-selectin EGF domain (P-sel:EGF) to examine the structure and function of this
domain independent of P-selectin. The peptide was folded in vitro and exhibited
the same disulfide bonding pattern as other EGF-like domains. P-sel:EGF did not
inhibit P-selectin-mediated cellular adhesion assays, indicating that the lectin
domain is also required. We undertook the study of the P-selectin EGF by 1H NMR
to determine its structure independent of the lectin domain and to compare its
structure to that of E-selectin determined crystallographically [Graves et al.
(1994) Nature 367, 532]. Although the binding of P-selectin to its carbohydrate
ligand is calcium dependent, and some EGF domains have calcium binding sites,
addition of calcium had no effect on the NMR spectrum or on the pH-induced
changes. Nearly complete resonance assignments were made from 2D 1H NMR spectra
at pH 6.0. Two sections of antiparallel beta-sheet were identified on the basis
of the pattern of long-range NOEs, 3JHN alpha coupling constants, and slowly
exchanging amides. The solution structure of the peptide backbone was determined
using distance geometry and simulated annealing calculations. The backbone RMSD
to the geometric average for 19 final structures is 0.64 +/- 0.17 A. The
resulting fold closely resembles that of other EGF-like peptides, including the
E-selectin EGF domain (RMSD approximately 1.08 A). However, compared to the
E-selectin EGF structure which also contains the lectin domain, some residues
from 1-11 are less ordered, and novel contacts occur between the amino terminus
and the core beta-sheet. Despite marked structural homology of the selectin
polypeptide backbones, the selectin EGF surfaces show unique distributions of
charged residues, a feature that likely correlates to the functional differences.
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