A loop region of BAFF controls B cell survival and regulates recognition by different inhibitors

Chambers, Melissa G.; Chevalley, Dehlia; Das, Dolon; Eslami, Mahya; Fomekong Nanfack, Yves; Hess, Henry; Hummler, Edith; Jiang, Xuliang; Kowalczyk-Quintas, Christine; Lammens, Alfred; Liao, Maofu; Mackay, Fabienne; Maskos, Klaus; Rolink, Antonius; Samy, Eileen; Schneider, Pascal; Schuepbach-Mallepell, Sonia; Smulski, Cristian R.; Tardivel, Aubry; Vigolo, Michele; Willen, Laure

A loop region of BAFF controls B cell survival and regulates recognition by different inhibitors

Authors: Melissa G. Chambers
Dehlia Chevalley
Dolon Das
Mahya Eslami
Yves Fomekong Nanfack
Henry Hess
Edith Hummler
Xuliang Jiang
Christine Kowalczyk-Quintas
Alfred Lammens
Maofu Liao
Fabienne Mackay
Klaus Maskos
Antonius Rolink
Eileen Samy
Pascal Schneider
Sonia Schuepbach-Mallepell
Cristian R. Smulski
Aubry Tardivel
Michele Vigolo
Laure Willen
Publication date: 23 March 2018
Publisher: 'Springer Science and Business Media LLC'
Doi

Abstract

The B cell survival factor (TNFSF13B/BAFF) is often elevated in autoimmune diseases and is targeted in the clinic for the treatment of systemic lupus erythematosus. BAFF contains a loop region designated the flap, which is dispensable for receptor binding. Here we show that the flap of BAFF has two functions. In addition to facilitating the formation of a highly active BAFF 60-mer as shown previously, it also converts binding of BAFF to TNFRSF13C (BAFFR) into a signaling event via oligomerization of individual BAFF-BAFFR complexes. Binding and activation of BAFFR can therefore be targeted independently to inhibit or activate the function of BAFF. Moreover, structural analyses suggest that the flap of BAFF 60-mer temporarily prevents binding of an anti-BAFF antibody (belimumab) but not of a decoy receptor (atacicept). The observed differences in profiles of BAFF inhibition may confer distinct biological and clinical efficacies to these therapeutically relevant inhibitors