Litcius/Paper detail

The therapeutic potential of sialylated Fc domains of human IgG

Richard J. Pleass

2021mAbs21 citationsDOIOpen Access PDF

Abstract

Pathogens frequently use multivalent binding to sialic acid to infect cells or to modulate immunity through interactions with human sialic acid-binding immunoglobulin-type lectins (Siglecs). Molecules that interfere with these interactions could be of interest as diagnostics, anti-infectives or as immune modulators. This review describes the development of molecular scaffolds based on the crystallizable fragment (Fc) region of immunoglobulin (Ig) G that deliver high-avidity binding to innate immune receptors, including sialic acid-dependent receptors. The ways in which the sialylated Fc may be engineered as immune modulators that mimic the anti-inflammatory properties of intravenous polyclonal Ig or as blockers of sialic-acid-dependent infectivity by viruses are also discussed.

Topics & Concepts

Sialic acidAvidityAntibodyFragment crystallizable regionSIGLECReceptorPolyclonal antibodiesImmune systemImmunoglobulin GGlycanImmunoglobulin Fc FragmentsInnate immune systemChemistryOpsoninFc receptorN-Acetylneuraminic acidCD22BiologyBiochemistryGlycoproteinImmunologyMonoclonal antibodyMonoclonal and Polyclonal Antibodies ResearchGlycosylation and Glycoproteins ResearchGalectins and Cancer Biology