Identification of a Novel Carbohydrate-Mimicking Octapeptide from Chemical Peptide Library and Characterization as Selectin Inhibitor

抄録

We found a novel octapeptide (H-YRNWFGRW-NH₂) mimicking sialyl Lewis X (sLe^X) carbohydrate from a chemical peptide library with anti-sLe^X monoclonal antibody (MAb) 2H5. The peptide libraries were constructed by Fmoc-based solid-phase methodology using the mix-split method. The octapeptide sequence was determined by the iterative deconvolution method using anti-sLe^X MAb 2H5. To define the important residues for interaction with anti-sLe^X MAb 2H5, alanine-scanning analogues of H-YRNWFGRW-NH₂ were synthesized. Substitution of Tyr¹, Trp⁴, Arg⁷ and Trp⁸ to Ala resulted in a marked drop in affinity. This result indicates that aromatic and cationic amino residues have a key role in interacting with anti-sLe^X MAb 2H5. The binding property of the octapeptide was evaluated with anti-sLe^X MAb 2H5 and human E-selectin. The octapeptide showed high inhibitory potency (IC₅₀=17.8 nM) for sLe^X and competitively inhibited the binding of anti-sLe^X MAb 2H5 in a dose-dependent manner. The octapeptide had high affinity (K_d=0.168 μM) for E-selectin and this binding was inhibited by sLe^X. These results suggest that octapeptide binds to anti-sLe^X MAb 2H5 or E-selectin at the sLe^X binding site and sterically interferes with the recognition of anti-sLe^X MAb 2H5 or E-selectin with sLe^X. This peptide may be a useful lead compound for an anti-inflammatory agent targeting selectin.