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Ligation of human Fc receptor like-2 by monoclonal antibodies down-regulates B-cell receptor-mediated signalling.

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posted on 2024-10-29, 12:22 authored by Mahdi Shabani, Ali Ahmad Bayat, Mahmood Jeddi-Tehrani, Hodjatallah Rabbani, Mohammad Hojjat-Farsangi, Cristina Ulivieri, Zahra Amirghofran, Cosima Tatiana Baldari, Fazel Shokri
B-cell antigen receptor (BCR) signalling and its regulation through negative and positive regulators are critical for balancing B-cell response and function. Human Fc receptor like-2 (FCRL2), a member of the newly identified FCRL family, could influence B-cell signalling due to possession of both immunoreceptor tyrosine-based activation and inhibitory motifs (ITAM and ITIM). Since the natural ligand of FCRL2 has not been identified, we generated FCRL2-specific monoclonal antibodies (mAbs) and employed them to investigate the influence of FCRL2 stimulation on BCR signalling in an FCRL2-expressing B-cell line. Two anti-FCRL2 mAb-producing hybridoma clones (5A7-E7 and 3D8-G8) were selected. None of the mAbs displayed any cross-reactivity with the other members of the FCRL family including recombinant FCRL1, -3, -4 and -5, as tested by FACS and ELISA techniques. Engagement of the FCRL2 by these mAbs resulted in significant inhibition of BCR signalling mediators such as calcium mobilization and phosphorylation of the mitogen-activated protein kinases Erk, p38 and Jnk. These findings indicate that the FCRL2 ITIM motifs are functional and the anti-FCRL2 mAbs may mimic the natural ligand of FCRL2 by induction of inhibitory signals in B cells.

History

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  • Accepted manuscript

Publication status

Published

Sub type

Article

Journal

Immunology

ISSN

0019-2805

eISSN

1365-2567

Volume

143

Issue

3

Pagination

341-353

Language

  • eng

Original self archiving date

2014-05-27

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