| Literature DB >> 30158170 |
Paul-Gydeon Ritvo1, Ahmed Saadawi1, Pierre Barennes1, Valentin Quiniou1,2, Wahiba Chaara1,2, Karim El Soufi1, Benjamin Bonnet1, Adrien Six1,2, Mikhail Shugay3,4,5, Encarnita Mariotti-Ferrandiz1,2, David Klatzmann6,2.
Abstract
T follicular helper (Tfh) and regulatory (Tfr) cells are terminally differentiated cells found in germinal centers (GCs), specialized secondary lymphoid organ structures dedicated to antibody production. As such, follicular T (Tfol) cells are supposed to be specific for immunizing antigens, which has been reported for Tfh cells but is debated for Tfr cells. Here, we used high-throughput T cell receptor (TCR) sequencing to analyze the repertoires of Tfh and Tfr cells, at homeostasis and after immunization with self- or foreign antigens. We observed that, whatever the conditions, Tfh and Tfr cell repertoires are less diverse than those of effector T cells and Treg cells of the same tissues; surprisingly, these repertoires still represent thousands of different sequences, even after immunization with a single antigen that induces a 10-fold increase in Tfol cell numbers. Thorough analysis of the sharing and network of TCR sequences revealed that a specific response to the immunizing antigen can only, but hardly, be detected in Tfh cells immunized with a foreign antigen and Tfr cells immunized with a self-antigen. These antigen-specific responses are obscured by a global stimulation of Tfh and Tfr cells that appears to be antigen-independent. Altogether, our results suggest a major bystander Tfol cell activation during the immune response in the GCs.Entities:
Keywords: TCR; autoimmunity; diversity; follicular; stochasticity
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Year: 2018 PMID: 30158170 PMCID: PMC6156623 DOI: 10.1073/pnas.1808594115
Source DB: PubMed Journal: Proc Natl Acad Sci U S A ISSN: 0027-8424 Impact factor: 11.205