Galectin-8 Favors the Presentation of Surface-Tethered Antigens by Stabilizing the B Cell Immune Synapse
Author(s) -
Dorian Obino,
Luc Fetler,
Andrea Soza,
Odile Malbec,
Juan José Sáez,
Mariana Labarca,
Claudia Oyanadel,
Felipe Del Valle Batalla,
Nicolas Goles,
Aleksandra Chikina,
Danielle Lankar,
Fabián SegoviaMiranda,
Camille Garcia,
Thibaut Léger,
Alfonso González,
Marion Espéli,
Ana-María Len-Duménil,
María-Isabel Yuseff
Publication year - 2018
Publication title -
cell reports
Language(s) - English
Resource type - Journals
SCImago Journal Rank - 6.264
H-Index - 154
eISSN - 2639-1856
pISSN - 2211-1247
DOI - 10.1016/j.celrep.2018.11.052
Subject(s) - microbiology and biotechnology , antigen , immunological synapse , antigen presentation , secretion , immune system , glycan , biology , extracellular matrix , extracellular , galectin 1 , chemistry , t cell , immunology , biochemistry , t cell receptor , glycoprotein
Complete activation of B cells relies on their capacity to extract tethered antigens from immune synapses by either exerting mechanical forces or promoting their proteolytic degradation through lysosome secretion. Whether antigen extraction can also be tuned by local cues originating from the lymphoid microenvironment has not been investigated. We here show that the expression of Galectin-8-a glycan-binding protein found in the extracellular milieu, which regulates interactions between cells and matrix proteins-is increased within lymph nodes under inflammatory conditions where it enhances B cell arrest phases upon antigen recognition in vivo and promotes synapse formation during BCR recognition of immobilized antigens. Galectin-8 triggers a faster recruitment and secretion of lysosomes toward the B cell-antigen contact site, resulting in efficient extraction of immobilized antigens through a proteolytic mechanism. Thus, extracellular cues can determine how B cells sense and extract tethered antigens and thereby tune B cell responses in vivo.
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