TY - JOUR
T1 - A novel unconventional T cell population enriched in Crohn's disease
AU - Rosati, Elisa
AU - Martini, Gabriela Rios
AU - Pogorelyy, Mikhail V.
AU - Minervina, Anastasia A.
AU - Degenhardt, Frauke
AU - Wendorff, Mareike
AU - Sari, Soner
AU - Mayr, Gabriele
AU - Fazio, Antonella
AU - Dowds, Christel Marie
AU - Hauser, Charlotte
AU - Tran, Florian
AU - von Schönfels, Witigo
AU - Pochhammer, Julius
AU - Salnikova, Maria A.
AU - Jaeckel, Charlot
AU - Gigla, Johannes Boy
AU - Sabet, Sanaz Sedghpour
AU - Hübenthal, Matthias
AU - Schiminsky, Esther
AU - Schreiber, Stefan
AU - Rosenstiel, Philip C.
AU - Scheffold, Alexander
AU - Thomas, Paul G.
AU - Lieb, Wolfgang
AU - Bokemeyer, Bernd
AU - Witte, Maria
AU - Aden, Konrad
AU - Hendricks, Alexander
AU - Schafmayer, Clemens
AU - Egberts, Jan Hendrick
AU - Mamedov, Ilgar Z.
AU - Bacher, Petra
AU - Franke, Andre
N1 - Publisher Copyright:
© 2022 Author(s) (or their employer(s)).
PY - 2022
Y1 - 2022
N2 - Objective: One of the current hypotheses to explain the proinflammatory immune response in IBD is a dysregulated T cell reaction to yet unknown intestinal antigens. As such, it may be possible to identify disease-associated T cell clonotypes by analysing the peripheral and intestinal T-cell receptor (TCR) repertoire of patients with IBD and controls. Design: We performed bulk TCR repertoire profiling of both the TCR alpha and beta chains using high-throughput sequencing in peripheral blood samples of a total of 244 patients with IBD and healthy controls as well as from matched blood and intestinal tissue of 59 patients with IBD and disease controls. We further characterised specific T cell clonotypes via single-cell RNAseq. Results: We identified a group of clonotypes, characterised by semi-invariant TCR alpha chains, to be significantly enriched in the blood of patients with Crohn's disease (CD) and particularly expanded in the CD8+ T cell population. Single-cell RNAseq data showed an innate-like phenotype of these cells, with a comparable gene expression to unconventional T cells such as mucosal associated invariant T and natural killer T (NKT) cells, but with distinct TCRs. Conclusions: We identified and characterised a subpopulation of unconventional Crohn-associated invariant T (CAIT) cells. Multiple evidence suggests these cells to be part of the NKT type II population. The potential implications of this population for CD or a subset thereof remain to be elucidated, and the immunophenotype and antigen reactivity of CAIT cells need further investigations in future studies.
AB - Objective: One of the current hypotheses to explain the proinflammatory immune response in IBD is a dysregulated T cell reaction to yet unknown intestinal antigens. As such, it may be possible to identify disease-associated T cell clonotypes by analysing the peripheral and intestinal T-cell receptor (TCR) repertoire of patients with IBD and controls. Design: We performed bulk TCR repertoire profiling of both the TCR alpha and beta chains using high-throughput sequencing in peripheral blood samples of a total of 244 patients with IBD and healthy controls as well as from matched blood and intestinal tissue of 59 patients with IBD and disease controls. We further characterised specific T cell clonotypes via single-cell RNAseq. Results: We identified a group of clonotypes, characterised by semi-invariant TCR alpha chains, to be significantly enriched in the blood of patients with Crohn's disease (CD) and particularly expanded in the CD8+ T cell population. Single-cell RNAseq data showed an innate-like phenotype of these cells, with a comparable gene expression to unconventional T cells such as mucosal associated invariant T and natural killer T (NKT) cells, but with distinct TCRs. Conclusions: We identified and characterised a subpopulation of unconventional Crohn-associated invariant T (CAIT) cells. Multiple evidence suggests these cells to be part of the NKT type II population. The potential implications of this population for CD or a subset thereof remain to be elucidated, and the immunophenotype and antigen reactivity of CAIT cells need further investigations in future studies.
UR - http://www.scopus.com/inward/record.url?scp=85137198012&partnerID=8YFLogxK
U2 - 10.1136/gutjnl-2021-325373
DO - 10.1136/gutjnl-2021-325373
M3 - Article
C2 - 35264446
AN - SCOPUS:85137198012
SN - 0017-5749
VL - 71
SP - 2194
EP - 2204
JO - Gut
JF - Gut
IS - 11
ER -