GMI-1070, a novel pan-selectin antagonist, reverses acute vascular occlusions in sickle cell mice

Author:

Chang Jungshan1,Patton John T.2,Sarkar Arun2,Ernst Beat3,Magnani John L.2,Frenette Paul S.1

Affiliation:

1. Departments of Medicine and Gene and Cell Medicine, Mount Sinai School of Medicine, New York, NY;

2. GlycoMimetics Inc, Gaithersburg, MD; and

3. Institute of Molecular Pharmacy, University of Basel, Basel, Switzerland

Abstract

Abstract Leukocyte adhesion in the microvasculature influences blood rheology and plays a key role in vaso-occlusive manifestations of sickle cell disease. Notably, polymorphonuclear neutrophils (PMNs) can capture circulating sickle red blood cells (sRBCs) in inflamed venules, leading to critical reduction in blood flow and vaso-occlusion. Recent studies have suggested that E-selectin expression by endothelial cells plays a key role by sending activating signals that lead to the activation of Mac-1 at the leading edge of PMNs, thereby allowing RBC capture. Thus, the inhibition of E-selectin may represent a valuable target in this disease. Here, we have tested the biologic properties of a novel synthetic pan-selectin inhibitor, GMI-1070, with in vitro assays and in a humanized model of sickle cell vaso-occlusion analyzed by intravital microscopy. We have found that GMI-1070 predominantly inhibited E-selectin–mediated adhesion and dramatically inhibited sRBC-leukocyte interactions, leading to improved microcirculatory blood flow and improved survival. These results suggest that GMI-1070 may represent a valuable novel therapeutic intervention for acute sickle cell crises that should be further evaluated in a clinical trial.

Publisher

American Society of Hematology

Subject

Cell Biology,Hematology,Immunology,Biochemistry

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