Litcius/Paper detail

SIGLEC-5/14 Inhibits CD11b/CD18 Integrin Activation and Neutrophil-Mediated Tumor Cell Cytotoxicity

Panagiota Bouti, Colin Blans, Bart Klein, Debarati Shome, Reza Nadafi, Michel van Houdt, Karin Schornagel, Paul J.J.H. Verkuijlen, Virginie Roos, Rogier M. Reijmers, Robin van Bruggen, Taco W. Kuijpers, Hanke L. Matlung

2023International Journal of Molecular Sciences13 citationsDOIOpen Access PDF

Abstract

Since the successful introduction of checkpoint inhibitors targeting the adaptive immune system, monoclonal antibodies inhibiting CD47-SIRPα interaction have shown promise in enhancing anti-tumor treatment efficacy. Apart from SIRPα, neutrophils express a broad repertoire of inhibitory receptors, including several members of the sialic acid-binding receptor (SIGLEC) family. Here, we demonstrate that interaction between tumor cell-expressed sialic acids and SIGLEC-5/14 on neutrophils inhibits antibody-dependent cellular cytotoxicity (ADCC). We observed that conjugate formation and trogocytosis, both essential processes for neutrophil ADCC, were limited by the sialic acid-SIGLEC-5/14 interaction. During neutrophil-tumor cell conjugate formation, we found that inhibition of the interaction between tumor-expressed sialic acids and SIGLEC-5/14 on neutrophils increased the CD11b/CD18 high affinity conformation. By dynamic acoustic force measurement, the binding between tumor cells and neutrophils was assessed. The interaction between SIGLEC-5/14 and the sialic acids was shown to inhibit the CD11b/CD18-regulated binding between neutrophils and antibody-opsonized tumor cells. Moreover, the interaction between sialic acids and SIGLEC-5/14-consequently hindered trogocytosis and tumor cell killing. In summary, our results provide evidence that the sialic acid-SIGLEC-5/14 interaction is an additional target for innate checkpoint blockade in the tumor microenvironment.

Topics & Concepts

SIGLECAntibody-dependent cell-mediated cytotoxicitySialic acidIntegrin alpha MMonoclonal antibodyBiologyReceptorCell biologyAntibodyOpsoninChemistryBiochemistryImmunologyPhagocytosis and Immune RegulationImmunotherapy and Immune ResponsesGlycosylation and Glycoproteins Research