CD8 T cells induce T-bet-dependent migration toward CXCR3 ligands by differentiated B cells produced during responses to alum-protein vaccines

Karine Serre*, Adam F. Cunningham, Ruth E. Coughlan, Andreia C. Lino, Antal Rot, Elin Hub, Katrin Moser, Rudolf Manz, Alastair Ferraro, Roger Bird, Kai Michael Toellner, Jocelyne Demengeot, Ian C.M. MacLennan, Elodie Mohr

*Korrespondierende/r Autor/-in für diese Arbeit
22 Zitate (Scopus)

Abstract

Antibody-forming cells (AFCs) expressing the chemokine receptor CXCR3 are recruited to sites of inflammation where they help clear pathogens but may participate in autoimmune diseases. Here we identify a mechanism that induces CXCR3 expression by AFC and germinal center (GC) B cells. This happens when CD8 T cells are recruited into CD4 T cell-dependent B-cell responses. Ovalbumin-specific CD4 T cells (OTII) were transferred alone or with ovalbumin-specific CD8 T cells (OTI) and the response to subcutaneous alum-precipitated ovalbumin was followed in the draining lymph nodes. OTII cells alone induce T helper 2-associated class switching to IgG1, but fewAFC or GC B cells express CXCR3. By contrast, OTI-derived IFN-γ induces most responding GC B cells and AFCs to express high levels of CXCR3, and diverse switching to IgG2a, IgG2b, with some IgG1. Up-regulation of CXCR3 by GC B cells and AFCs and their migration toward its ligand CXCL10 are shown to depend on B cells' intrinsic T-bet, a transcription factor downstream of the IFN-γR signaling. This model clarifies how precursors of long-lived AFCs and memory B cells acquire CXCR3 that causes their migration to inflammatory foci.

OriginalspracheEnglisch
ZeitschriftBlood
Jahrgang120
Ausgabenummer23
Seiten (von - bis)4552-4559
Seitenumfang8
ISSN0006-4971
DOIs
PublikationsstatusVeröffentlicht - 29.11.2012

Strategische Forschungsbereiche und Zentren

  • Forschungsschwerpunkt: Infektion und Entzündung - Zentrum für Infektions- und Entzündungsforschung Lübeck (ZIEL)

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