PT - JOURNAL ARTICLE AU - Johansson, David AU - Rauld, Céline AU - Roux, Julien AU - Regairaz, Camille AU - Galli, Edoardo AU - Callegari, Ilaria AU - Raad, Layla AU - Waldt, Annick AU - Cuttat, Rachel AU - Roma, Guglielmo AU - Diebold, Martin AU - Becher, Burkhard AU - Kuhle, Jens AU - Derfuss, Tobias AU - Carballido, José M. AU - Sanderson, Nicholas S.R. TI - Mass Cytometry of CSF Identifies an MS-Associated B-cell Population AID - 10.1212/NXI.0000000000000943 DP - 2021 Mar 01 TA - Neurology - Neuroimmunology Neuroinflammation PG - e943 VI - 8 IP - 2 4099 - http://nn.neurology.org/content/8/2/e943.short 4100 - http://nn.neurology.org/content/8/2/e943.full SO - Neurol Neuroimmunol Neuroinflamm2021 Mar 01; 8 AB - Objective To identify an MS-specific immune cell population by deep immune phenotyping and relate it to soluble signaling molecules in CSF.Methods We analyzed surface expression of 22 markers in paired blood/CSF samples from 39 patients using mass cytometry (cytometry by time of flight). We also measured the concentrations of 296 signaling molecules in CSF using proximity extension assay. Results were analyzed using highly automated unsupervised algorithmic informatics.Results Mass cytometry objectively identified a B-cell population characterized by the expression of CD49d, CD69, CD27, CXCR3, and human leukocyte antigen (HLA)-DR as clearly associated with MS. Concentrations of the B cell–related factors, notably FCRL2, were increased in MS CSF, especially in early stages of the disease. The B-cell trophic factor B cell activating factor (BAFF) was decreased in MS. Proteins involved in neural plasticity were also reduced in MS.Conclusion When analyzed without a priori assumptions, both the soluble and the cellular compartments of the CSF in MS were characterized by markers related to B cells, and the strongest candidate for an MS-specific cell type has a B-cell phenotype.BSA=bovine serum albumin; CyTOF=cytometry by time of flight; FDR=false discovery rate; ICOS=inducible T-cell costimulator; PCA=principal component analysis; PEA=proximal extension assay; PBMC=peripheral blood mononuclear cell; PBS=phosphate-buffered saline