Deconvolution of B cell receptor repertoire in multiple sclerosis patients revealed a delay in tBreg maturation.

BACKGROUND

B lymphocytes play a pivotal regulatory role in the development of the immune response. It was previously shown that deficiency in B regulatory cells (Bregs) or a decrease in their anti-inflammatory activity can lead to immunological dysfunctions. However, the exact mechanisms of Bregs development and functioning are only partially resolved. For instance, only a little is known about the structure of their B cell receptor (BCR) repertoires in autoimmune disorders, including multiple sclerosis (MS), a severe neuroinflammatory disease with a yet unknown etiology. Here, we elucidate specific properties of B regulatory cells in MS.

METHODS

We performed a prospective study of the transitional Breg (tBreg) subpopulations with the CD19CD24CD38 phenotype from MS patients and healthy donors by (i) measuring their content during two diverging courses of relapsing-remitting MS: benign multiple sclerosis (BMS) and highly active multiple sclerosis (HAMS); (ii) analyzing BCR repertoires of circulating B cells by high-throughput sequencing; and (iii) measuring the percentage of CD27 cells in tBregs.

RESULTS

The tBregs from HAMS patients carry the heavy chain with a lower amount of hypermutations than tBregs from healthy donors. The percentage of transitional CD24CD38 B cells is elevated, whereas the frequency of differentiated CD27 cells in this transitional B cell subset was decreased in the MS patients as compared with healthy donors.

CONCLUSIONS

Impaired maturation of regulatory B cells is associated with MS progression.