Sialyl Lewisx (sLex) and an sLexMimetic, CGP69669A, Disrupt E-Selectin–Dependent Leukocyte Rolling In Vivo

Author:

Norman Keith E.1,Anderson Gary P.1,Kolb Hartmut C.1,Ley Klaus1,Ernst Beat1

Affiliation:

1. From the Departments of Transplantation and Respiratory Diseases, Novartis AG, Basle, Switzerland; and the Department of Biomedical Engineering, University of Virginia Health Sciences Center, Charlottesville, VA

Abstract

AbstractLeukocyte rolling is the earliest observable event in their recruitment from the circulation to inflamed tissue. This rolling is mediated largely by interaction between the selectin family of adhesion molecules and their glycosylated ligands. Although the nature of these ligands and their interaction with the selectins is not fully understood, it is accepted that expression of fucosylated sialylated glycans such as sialyl Lewisx (sLex) is required for function. Despite findings that sLex inhibits binding of leukocytes to E-selectin in vitro, and has beneficial effects in inflammatory disease models, inhibition of E-selectin–dependent leukocyte rolling in vivo has not been described. Functional overlap between the selectins has been noted and reduction of rolling by E-selectin antibodies only occurs if P-selectin is absent or blocked. We demonstrate that leukocyte rolling velocity in tumor necrosis factor alpha (TNFα)-stimulated mouse cremaster is increased following treatment with either sLex or the sLex-mimetic CGP69669A and that rolling is dramatically reduced if CGP69669A is applied in the presence of anti–P-selectin antibody. These effects are characteristic of E-selectin antagonism. In contrast, surgically stimulated (L- or P-selectin–dependent) rolling is unaffected by either sLex or CGP69669A. Our data demonstrate that CGP69669A is an effective and selective antagonist of E-selectin in vivo.

Publisher

American Society of Hematology

Subject

Cell Biology,Hematology,Immunology,Biochemistry

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1. E-selectin in vascular pathophysiology;Frontiers in Immunology;2024-07-19

2. A Structural-Reporter Group to Determine the Core Conformation of Sialyl Lewisx Mimetics;Molecules;2023-03-13

3. Glycomimetics for the inhibition and modulation of lectins;Chemical Society Reviews;2023

4. Novel approaches to glycomimetic design: development of small molecular weight lectin antagonists;Expert Opinion on Drug Discovery;2021-02-05

5. Sialic acid and biology of life: An introduction;Sialic Acids and Sialoglycoconjugates in the Biology of Life, Health and Disease;2020

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