Please use this identifier to cite or link to this item: http://hdl.handle.net/1942/37621
Title: Distinct Effector Programs of Brain-Homing CD8(+) T Cells in Multiple Sclerosis
Authors: Koetzier, Steven C.
van Langelaar, Jamie
Melief, Marie-Jose
Wierenga-Wolf, Annet F.
Corsten, Cato E. A.
Blok, Katelijn M.
HOEKS, Cindy 
BROUX, Bieke 
Wokke, Beatrijs
van Luijn, Marvin M.
Smolders, Joost
Issue Date: 2022
Publisher: MDPI
Source: Cells, 11 (10) (Art N° 1634)
Abstract: The effector programs of CD8(+) memory T cells are influenced by the transcription factors RUNX3, EOMES and T-bet. How these factors define brain-homing CD8(+) memory T cells in multiple sclerosis (MS) remains unknown. To address this, we analyzed blood, CSF and brain tissues from MS patients for the impact of differential RUNX3, EOMES and T-bet expression on CD8(+) T cell effector phenotypes. The frequencies of RUNX3- and EOMES-, but not T-bet-expressing CD8(+) memory T cells were reduced in the blood of treatment-naive MS patients as compared to healthy controls. Such reductions were not seen in MS patients treated with natalizumab (anti-VLA-4 Ab). We found an additional loss of T-bet in RUNX3-expressing cells, which was associated with the presence of MS risk SNP rs6672420 (RUNX3). RUNX3(+)EOMES(+)T-bet(-) CD8(+) memory T cells were enriched for the brain residency-associated markers CCR5, granzyme K, CD20 and CD69 and selectively dominated the MS CSF. In MS brain tissues, T-bet coexpression was recovered in CD20(dim) and CD69(+) CD8(+) T cells, and was accompanied by increased coproduction of granzyme K and B. These results indicate that coexpression of RUNX3 and EOMES, but not T-bet, defines CD8(+) memory T cells with a pre-existing brain residency-associated phenotype such that they are prone to enter the CNS in MS.
Notes: van Luijn, MM; Smolders, J (corresponding author), Erasmus MC, Dept Immunol, Univ Med Ctr Rotterdam, NL-3000 Rotterdam, Netherlands.; van Luijn, MM; Smolders, J (corresponding author), Erasmus MC, MS Ctr ErasMS, Univ Med Ctr Rotterdam, NL-3000 Rotterdam, Netherlands.; Smolders, J (corresponding author), Erasmus MC, Dept Neurol, Univ Med Ctr Rotterdam, NL-3000 Rotterdam, Netherlands.; Smolders, J (corresponding author), Netherlands Inst Neurosci, Neuroimmunol Res Grp, NL-1105 Amsterdam, Netherlands.
s.koetzier@erasmusmc.nl; j.vanlangelaar@erasmusmc.nl;
j.melief@erasmusmc.nl; a.wierenga-wolf@erasmusmc.nl;
c.corsten@erasmusmc.nl; k.blok@erasmusmc.nl; cindy.hoeks@uhasselt.be;
bieke.broux@uhasselt.be; b.wokke@erasmusmc.nl; m.vanluijn@erasmusmc.nl;
j.j.f.m.smolders@erasmusmc.nl
Keywords: transcription factors;cytotoxicity;pre-existing and brain-residency
Document URI: http://hdl.handle.net/1942/37621
e-ISSN: 2073-4409
DOI: 10.3390/cells11101634
ISI #: WOS:000801870000001
Rights: 2022 by the authors. Licensee MDPI, Basel, Switzerland. This article is an open access article distributed under the terms and conditions of the Creative Commons Attribution (CC BY) license (https:// creativecommons.org/licenses/by/ 4.0/)
Category: A1
Type: Journal Contribution
Validations: ecoom 2023
Appears in Collections:Research publications

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