Literature DB >> 24227819

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

Andrew T Vaughan1, 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.   

Abstract

A major feature that distinguishes type I from type II anti-CD20 monoclonal antibodies (mAbs) and reduces their therapeutic efficacy is the tendency to internalize from the cell surface. We have shown previously that the extent of internalization correlates with the capacity of type I mAb to simultaneously engage both CD20 and the inhibitory Fcγ receptor, FcγRIIb, in a bipolar configuration. Here, we investigated whether mAbs directed at other B-cell surface receptors also engaged FcγRIIb and whether this interaction promoted internalization. Most mAbs engaged and activated FcγRIIb, with the strength of activation related to the level of mAb bound to the cell surface. However, engagement did not affect internalization of most mAb-ligated receptors, either in cell lines or primary chronic lymphocytic leukemia cells with the exception of CD19 and CD38. Furthermore, at high cell concentrations/density both cis and trans interactions between cell-surface bound mAb and FcγRIIb were evident, but trans interactions did not inhibit type I anti-CD20 mAb-mediated internalization. These data identify that FcγRIIb is engaged by many mAbs in both cis and trans configurations, triggering its activation, but that internalization via FcγRIIb occurs for only a select subset. These findings have implications when designing new antibody-based therapeutics.

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Year:  2013        PMID: 24227819     DOI: 10.1182/blood-2013-04-490821

Source DB:  PubMed          Journal:  Blood        ISSN: 0006-4971            Impact factor:   22.113


  22 in total

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Journal:  Sci Transl Med       Date:  2021-04-14       Impact factor: 17.956

2.  Resistance is futile: Targeting the inhibitory FcγRIIB (CD32B) to maximize immunotherapy.

Authors:  Ali Roghanian; Mark S Cragg; Björn Frendéus
Journal:  Oncoimmunology       Date:  2015-08-12       Impact factor: 8.110

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Journal:  Nat Rev Cancer       Date:  2015-06       Impact factor: 60.716

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

Authors:  Andrew T Vaughan; Claude H T Chan; Christian Klein; Martin J Glennie; Stephen A Beers; Mark S Cragg
Journal:  J Biol Chem       Date:  2015-01-07       Impact factor: 5.157

5.  ImmunoPET of Malignant and Normal B Cells with 89Zr- and 124I-Labeled Obinutuzumab Antibody Fragments Reveals Differential CD20 Internalization In Vivo.

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Review 6.  Three major uncertainties in the antibody therapy of cancer.

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Review 7.  Influence of immunoglobulin isotype on therapeutic antibody function.

Authors:  Stephen A Beers; Martin J Glennie; Ann L White
Journal:  Blood       Date:  2016-01-13       Impact factor: 22.113

8.  Shaving Is an Epiphenomenon of Type I and II Anti-CD20-Mediated Phagocytosis, whereas Antigenic Modulation Limits Type I Monoclonal Antibody Efficacy.

Authors:  Lekh N Dahal; Chie-Yin Huang; Richard J Stopforth; Abbie Mead; Keith Chan; Juliet X Bowater; Martin C Taylor; Priyanka Narang; H T Claude Chan; Jinny H Kim; Andrew T Vaughan; Francesco Forconi; Stephen A Beers
Journal:  J Immunol       Date:  2018-07-11       Impact factor: 5.422

9.  Functional Interactions of Common Allotypes of Rhesus Macaque FcγR2A and FcγR3A with Human and Macaque IgG Subclasses.

Authors:  Michael W Grunst; Andres G Grandea; Sanath Kumar Janaka; Iman Hammad; Parker Grimes; Julie A Karl; Roger Wiseman; David H O'Connor; David T Evans
Journal:  J Immunol       Date:  2020-11-18       Impact factor: 5.422

10.  TNF receptor agonists induce distinct receptor clusters to mediate differential agonistic activity.

Authors:  Xiaojie Yu; Sonya James; James H Felce; Blanka Kellermayer; David A Johnston; H T Claude Chan; Christine A Penfold; Jinny Kim; Tatyana Inzhelevskaya; C Ian Mockridge; Yasunori Watanabe; Max Crispin; Ruth R French; Patrick J Duriez; Leon R Douglas; Martin J Glennie; Mark S Cragg
Journal:  Commun Biol       Date:  2021-06-23
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