Literature DB >> 25568316

Activatory and inhibitory Fcγ receptors augment rituximab-mediated internalization of CD20 independent of signaling via the cytoplasmic domain.

Andrew T Vaughan1, Claude H T Chan1, Christian Klein2, Martin J Glennie1, Stephen A Beers1, Mark S Cragg3.   

Abstract

Type I anti-CD20 mAb such as rituximab and ofatumumab engage with the inhibitory FcγR, FcγRIIb on the surface of B cells, resulting in immunoreceptor tyrosine-based inhibitory motif (ITIM) phosphorylation. Internalization of the CD20·mAb·FcγRIIb complex follows, the rate of which correlates with FcγRIIb expression. In contrast, although type II anti-CD20 mAb such as tositumomab and obinutuzumab also interact with and activate FcγRIIb, this interaction fails to augment the rate of CD20·mAb internalization, raising the question of whether ITIM phosphorylation plays any role in this process. We have assessed the molecular requirements for the internalization process and demonstrate that in contrast to internalization of IgG immune complexes, FcγRIIb-augmented internalization of rituximab-ligated CD20 occurs independently of the FcγRIIb ITIM, indicating that signaling downstream of FcγRIIb is not required. In transfected cells, activatory FcγRI, FcγRIIa, and FcγRIIIa augmented internalization of rituximab-ligated CD20 in a similar manner. However, FcγRIIa mediated a slower rate of internalization than cells expressing equivalent levels of the highly homologous FcγRIIb. The difference was maintained in cells expressing FcγRIIa and FcγRIIb lacking cytoplasmic domains and in which the transmembrane domains had been exchanged. This difference may be due to increased degradation of FcγRIIa, which traffics to lysosomes independently of rituximab. We conclude that the cytoplasmic domain of FcγR is not required for promoting internalization of rituximab-ligated CD20. Instead, we propose that FcγR provides a structural role in augmenting endocytosis that differs from that employed during the endocytosis of immune complexes.
© 2015 by The American Society for Biochemistry and Molecular Biology, Inc.

Entities:  

Keywords:  Antibody; B Cell; CD20; Cell Signaling; Fc-gamma Receptor; Lipid Raft; Lymphoma; Receptor Endocytosis

Mesh:

Substances:

Year:  2015        PMID: 25568316      PMCID: PMC4342459          DOI: 10.1074/jbc.M114.593806

Source DB:  PubMed          Journal:  J Biol Chem        ISSN: 0021-9258            Impact factor:   5.157


  35 in total

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Journal:  Blood       Date:  2002-09-19       Impact factor: 22.113

2.  Store-operated cation entry mediated by CD20 in membrane rafts.

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Journal:  J Biol Chem       Date:  2003-08-14       Impact factor: 5.157

3.  Antibody specificity controls in vivo effector mechanisms of anti-CD20 reagents.

Authors:  Mark S Cragg; Martin J Glennie
Journal:  Blood       Date:  2003-10-09       Impact factor: 22.113

4.  CD20-induced lymphoma cell death is independent of both caspases and its redistribution into triton X-100 insoluble membrane rafts.

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5.  The CD20 calcium channel is localized to microvilli and constitutively associated with membrane rafts: antibody binding increases the affinity of the association through an epitope-dependent cross-linking-independent mechanism.

Authors:  Haidong Li; Linda M Ayer; Maria J Polyak; Cathlin M Mutch; Ryan J Petrie; Laura Gauthier; Neda Shariat; Michael J Hendzel; Andrew R Shaw; Kamala D Patel; Julie P Deans
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6.  Characterization of a new monoclonal anti-Fc gamma RII antibody, AT10, and its incorporation into a bispecific F(ab')2 derivative for recruitment of cytotoxic effectors.

Authors:  J Greenman; A L Tutt; A J George; K A Pulford; G T Stevenson; M J Glennie
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7.  Preparation and performance of bispecific F(ab' gamma)2 antibody containing thioether-linked Fab' gamma fragments.

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8.  Tyrosine-containing sequence motifs of the human immunoglobulin G receptors FcRIIb1 and FcRIIb2 essential for endocytosis and regulation of calcium flux in B cells.

Authors:  P Budde; N Bewarder; V Weinrich; O Schulzeck; J Frey
Journal:  J Biol Chem       Date:  1994-12-02       Impact factor: 5.157

9.  Fc receptor endocytosis is controlled by a cytoplasmic domain determinant that actively prevents coated pit localization.

Authors:  H M Miettinen; K Matter; W Hunziker; J K Rose; I Mellman
Journal:  J Cell Biol       Date:  1992-02       Impact factor: 10.539

10.  Inhibitory FcγRIIb (CD32b) becomes activated by therapeutic mAb in both cis and trans and drives internalization according to antibody specificity.

Authors:  Andrew T Vaughan; Chisako Iriyama; Stephen A Beers; Claude H T Chan; Sean H Lim; Emily L Williams; Vallari Shah; Ali Roghanian; Bjorn Frendéus; Martin J Glennie; Mark S Cragg
Journal:  Blood       Date:  2013-11-13       Impact factor: 22.113

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  8 in total

1.  STIM1 knock-down decreases the affinity of obinutuzumab for CD20 by altering CD20 localization to Triton-soluble membrane.

Authors:  W Heo; N Jin; M S Park; H-Y Kim; S M Yoon; J Lee; J Y Kim
Journal:  Clin Exp Immunol       Date:  2020-02-21       Impact factor: 4.330

2.  Detection of Experimental and Clinical Immune Complexes by Measuring SHIP-1 Recruitment to the Inhibitory FcγRIIB.

Authors:  Richard J Stopforth; Robert J Oldham; Alison L Tutt; Patrick Duriez; H T Claude Chan; Brock F Binkowski; Chad Zimprich; Dun Li; Philip G Hargreaves; Mei Cong; Venkat Reddy; Maria J Leandro; Geraldine Cambridge; Anja Lux; Falk Nimmerjahn; Mark S Cragg
Journal:  J Immunol       Date:  2018-01-19       Impact factor: 5.422

3.  IgG Fc domains that bind C1q but not effector Fcγ receptors delineate the importance of complement-mediated effector functions.

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Journal:  Nat Immunol       Date:  2017-06-12       Impact factor: 25.606

Review 4.  Regulation of Monoclonal Antibody Immunotherapy by FcγRIIB.

Authors:  Richard J Stopforth; Kirstie L S Cleary; Mark S Cragg
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5.  Activating Autophagy Enhanced the Antitumor Effect of Antibody Drug Conjugates Rituximab-Monomethyl Auristatin E.

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Review 6.  The Human FcγRII (CD32) Family of Leukocyte FcR in Health and Disease.

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7.  Complement-Dependent Activity of CD20-Specific IgG Correlates With Bivalent Antigen Binding and C1q Binding Strength.

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8.  Monitoring of the Complement System Status in Patients With B-Cell Malignancies Treated With Rituximab.

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  8 in total

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