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Fc gamma receptor IIb on target B cells promotes rituximab internalization and reduces clinical efficacy

Fc gamma receptor IIb on target B cells promotes rituximab internalization and reduces clinical efficacy
Fc gamma receptor IIb on target B cells promotes rituximab internalization and reduces clinical efficacy
The anti-CD20 mAb rituximab is central to the treatment of B-cell malignancies, but resistance remains a significant problem. We recently reported that resistance could be explained, in part, by internalization of rituximab (type I anti-CD20) from the surface of certain B-cell malignancies, thus limiting engagement of natural effectors and increasing mAb consumption. Internalization of rituximab was most evident in chronic lymphocytic leukemia (CLL) and mantle cell lymphoma (MCL), but the extent of internalization was heterogeneous within each disease. Here, we show that the inhibitory Fc?RIIb on target B cells promotes this process and is largely responsible for the observed heterogeneity across a range of B-cell malignancies. Internalization correlated strongly with Fc?RIIb expression on normal and malignant B cells, and resulted in reduced macrophage phagocytosis of mAb-coated targets. Furthermore, transfection of Fc?RIIb into Fc?RIIb negative Ramos cells increased internalization of rituximab in a dose-dependent manner. Target-cell Fc?RIIb promoted rituximab internalization in a cis fashion and was independent of Fc?RIIb on neighboring cells. It became phosphorylated and internalized along with CD20:anti-CD20 complexes before lysosomal degradation. In MCL patients, high Fc?RIIb expression predicted less durable responses after rituximab-containing regimens. Therefore, target-cell Fc?RIIb provides a potential biomarker of response to type I anti-CD20 mAb
0006-4971
2530-2540
Lim, Sean
1afe5aa1-61a4-4a7b-927f-5e671f885196
Vaughan, Andrew
bfb2ceab-a592-457e-89f9-00fcd1dddbdb
Ashton-Key, Margaret
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Williams, E.L.
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Dixon, S.
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Chan, H.T. Claude
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Beers, Stephen
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French, R.R.
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Cox, K.
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Davies, A.J.
0fe6a40a-10d1-4ade-a7e6-d1dceb2470af
Potter, Kathleen N.
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Mockridge, C.I.
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Oscier, David G.
c2620a1d-25bb-48f7-9651-f5d023636381
Johnson, P.W.M.
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Cragg, Mark
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Glennie, Martin
9f6f0eff-4560-48c2-80cd-0ec116110ded
Lim, Sean
1afe5aa1-61a4-4a7b-927f-5e671f885196
Vaughan, Andrew
bfb2ceab-a592-457e-89f9-00fcd1dddbdb
Ashton-Key, Margaret
5994ca63-021e-44b1-86c4-b7ae53321101
Williams, E.L.
08adaeea-f0e2-4ae5-a46d-fc9e515e7e8e
Dixon, S.
2f5e5170-8912-40af-8069-c4868e9aa1d3
Chan, H.T. Claude
b109c93f-7e9a-44ee-ad12-da757b1b11fc
Beers, Stephen
a02548be-3ffd-41ab-9db8-d6e8c3b499a2
French, R.R.
a95ea7a1-7aeb-4c20-998e-fde663613fd1
Cox, K.
7305c27e-9cdc-4e37-b994-ac55d7d1dfd2
Davies, A.J.
0fe6a40a-10d1-4ade-a7e6-d1dceb2470af
Potter, Kathleen N.
86a99047-494b-405b-a3f7-650c1dcd5838
Mockridge, C.I.
327aef17-4837-4f2a-a93b-3d17cd1a7f9f
Oscier, David G.
c2620a1d-25bb-48f7-9651-f5d023636381
Johnson, P.W.M.
3f6068ce-171e-4c2c-aca9-dc9b6a37413f
Cragg, Mark
ec97f80e-f3c8-49b7-a960-20dff648b78c
Glennie, Martin
9f6f0eff-4560-48c2-80cd-0ec116110ded

Lim, Sean, Vaughan, Andrew, Ashton-Key, Margaret, Williams, E.L., Dixon, S., Chan, H.T. Claude, Beers, Stephen, French, R.R., Cox, K., Davies, A.J., Potter, Kathleen N., Mockridge, C.I., Oscier, David G., Johnson, P.W.M., Cragg, Mark and Glennie, Martin (2011) Fc gamma receptor IIb on target B cells promotes rituximab internalization and reduces clinical efficacy. Blood, 118 (9), 2530-2540. (doi:10.1182/blood-2011-01-330357). (PMID:21768293)

Record type: Article

Abstract

The anti-CD20 mAb rituximab is central to the treatment of B-cell malignancies, but resistance remains a significant problem. We recently reported that resistance could be explained, in part, by internalization of rituximab (type I anti-CD20) from the surface of certain B-cell malignancies, thus limiting engagement of natural effectors and increasing mAb consumption. Internalization of rituximab was most evident in chronic lymphocytic leukemia (CLL) and mantle cell lymphoma (MCL), but the extent of internalization was heterogeneous within each disease. Here, we show that the inhibitory Fc?RIIb on target B cells promotes this process and is largely responsible for the observed heterogeneity across a range of B-cell malignancies. Internalization correlated strongly with Fc?RIIb expression on normal and malignant B cells, and resulted in reduced macrophage phagocytosis of mAb-coated targets. Furthermore, transfection of Fc?RIIb into Fc?RIIb negative Ramos cells increased internalization of rituximab in a dose-dependent manner. Target-cell Fc?RIIb promoted rituximab internalization in a cis fashion and was independent of Fc?RIIb on neighboring cells. It became phosphorylated and internalized along with CD20:anti-CD20 complexes before lysosomal degradation. In MCL patients, high Fc?RIIb expression predicted less durable responses after rituximab-containing regimens. Therefore, target-cell Fc?RIIb provides a potential biomarker of response to type I anti-CD20 mAb

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More information

Published date: 1 September 2011
Organisations: Cancer Sciences

Identifiers

Local EPrints ID: 339294
URI: http://eprints.soton.ac.uk/id/eprint/339294
DOI: doi:10.1182/blood-2011-01-330357
ISSN: 0006-4971
PURE UUID: 0f753199-244e-40cf-9488-ec9919e7e430
ORCID for Andrew Vaughan: ORCID iD orcid.org/0000-0001-6076-3649
ORCID for H.T. Claude Chan: ORCID iD orcid.org/0000-0003-0530-9480
ORCID for Stephen Beers: ORCID iD orcid.org/0000-0002-3765-3342
ORCID for A.J. Davies: ORCID iD orcid.org/0000-0002-7517-6938
ORCID for P.W.M. Johnson: ORCID iD orcid.org/0000-0003-2306-4974
ORCID for Mark Cragg: ORCID iD orcid.org/0000-0003-2077-089X

Catalogue record

Date deposited: 28 May 2012 13:53
Last modified: 15 Mar 2024 03:31

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Contributors

Author: Sean Lim
Author: Andrew Vaughan ORCID iD
Author: Margaret Ashton-Key
Author: E.L. Williams
Author: S. Dixon
Author: H.T. Claude Chan ORCID iD
Author: Stephen Beers ORCID iD
Author: R.R. French
Author: K. Cox
Author: A.J. Davies ORCID iD
Author: Kathleen N. Potter
Author: C.I. Mockridge
Author: David G. Oscier
Author: P.W.M. Johnson ORCID iD
Author: Mark Cragg ORCID iD
Author: Martin Glennie

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