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Association of IgG1 Antibody Clearance with FcγRIIA Polymorphism and Platelet Count in Infliximab-Treated Patients
Authors:Gilles Thibault  Gilles Paintaud  Hsueh Cheng Sung  Laurie Lajoie  Edouard Louis  the GETAID  Celine Desvignes  Herv Watier  Valrie Gouilleux-Gruart  David Ternant
Affiliation:1.EA 7501 GICC, Université de Tours, 37032 Tours, France; (G.P.); (H.C.S.); (L.L.); (C.D.); (H.W.); (V.G.-G.); (D.T.);2.Laboratoire d’Immunologie, CHRU de Tours, 37032 Tours, France;3.Laboratoire de Pharmacologie-Toxicologie, CHRU de Tours, 37044 Tours, France;4.Department of Gastroenterology, University Hospital, CHU of Liège, 4000 Liège, Belgium;
Abstract:The FcγRIIA/CD32A is mainly expressed on platelets, myeloid and several endothelial cells. Its affinity is considered insufficient for allowing significant binding of monomeric IgG, while its H131R polymorphism (histidine > arginine at position 131) influences affinity for multimeric IgG2. Platelet FcγRIIA has been reported to contribute to IgG-containing immune-complexe clearance. Given our finding that platelet FcγRIIA actually binds monomeric IgG, we investigated the role of platelets and FcγRIIA in IgG antibody elimination. We used pharmacokinetics analysis of infliximab (IgG1) in individuals with controlled Crohn’s disease. The influence of platelet count and FcγRIIA polymorphism was quantified by multivariate linear modelling. The infliximab half-life increased with R allele number (13.2, 14.4 and 15.6 days for HH, HR and RR patients, respectively). It decreased with increasing platelet count in R carriers: from ≈20 days (RR) and ≈17 days (HR) at 150 × 109/L, respectively, to ≈13 days (both HR and RR) at 350 × 109/L. Moreover, a flow cytometry assay showed that infliximab and monomeric IgG1 bound efficiently to platelet FcγRIIA H and R allotypes, whereas panitumumab and IgG2 bound poorly to the latter. We propose that infliximab (and presumably any IgG1 antibody) elimination is partly due to an unappreciated mechanism dependent on binding to platelet FcγRIIA, which is probably tuned by its affinity for IgG2.
Keywords:Fcγ  RIIA  polymorphism  platelets  Fc–  Fc receptor interaction  immunotherapy  monoclonal antibodies  clearance  IgG subclasses
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