| Article ID | Journal | Published Year | Pages | File Type |
|---|---|---|---|---|
| 3352980 | Immunity | 2014 | 14 Pages |
•CTLA-4 inhibits Tfh and Tfr cell differentiation and/or maintenance•Treg and/or Tfr cells suppress extrafollicular B cell B7-2 expression•CTLA-4 inhibits Tfh stimulation of B cell responses•Tfr cells suppress GC B cells through CTLA-4, but not by altering B7-2 levels
SummaryThe receptor CTLA-4 has been implicated in controlling B cell responses, but the mechanisms by which CTLA-4 regulates antibody production are not known. Here we showed deletion of CTLA-4 in adult mice increased Tfh and Tfr cell numbers and augmented B cell responses. In the effector phase, loss of CTLA-4 on Tfh cells resulted in heightened B cell responses, whereas loss of CTLA-4 on Tfr cells resulted in defective suppression of antigen-specific antibody responses. We also found that non-Tfr Treg cells could suppress B cell responses through CTLA-4 and that Treg and/or Tfr cells might downregulate B7-2 on B cells outside germinal centers as a means of suppression. Within the germinal center, however, Tfr cells potently suppress B cells through CTLA-4, but with a mechanism independent of altering B7-1 or B7-2. Thus, we identify multifaceted regulatory roles for CTLA-4 in Tfh, Tfr, and Treg cells, which together control humoral immunity.
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