B cell subpopulations in the pathogenesis of rheumatoid arthritis
Abstract
B cell depleting therapy has proven to be an effective treatment in rheumatoid arthritis (RA), a disease characterized by the presence of autoantibodies against citrullinated proteins (ACPA) and the Fc portion of IgG (rheumatoid factor, RF). This demonstrates the vital role B cells play in the disease. The aim of this thesis was to explore the role of B cell subpopulations in the pathogenesis of RA. Our interest in a specific B cell population arose with the discovery of murine autoreactive B cells, CD21-/low cells, which expressed low surface levels or lacked the complement receptor 2 (CD21). CD21 helps activate B cells, as it is a part of the B cell co-receptor complex.
In Studies I-III we analyzed B cell populations in human peripheral blood with the help of flow cytometry utilizing multiple cell markers. In Studies II-III, clinical as well as radiographic data was collected from RA patients.
In Study I we established that CD21-/low B cells are found in human peripheral blood and discovered that in healthy donors (HDs) this B cell population is mainly composed of memory B cells (MBCs) based on their phenotype and response to combined stimuli. In Study II we compared the B cell populations in peripheral blood of patients with established RA and HDs. We saw a higher proportion of a CD21-/low subpopulation, i.e. CD21-/low CD27-IgD- (double negative, DN) in patients with autoantibodies (ACPA/RF) compared to HDs. Additionally, the frequency of CD21- /low DN cells was higher in ACPA/RF positive patients with more joint destruction compared to those with less, and the CD21-/low DN population correlated positively with the level of destruction. The CD21-/low DN population was highly enriched in the inflamed joints of RA patients and a third of the cells expressed RANKL, which stimulates osteoclastogenesis. In Study III, we compared the B cell populations in peripheral blood in newly diagnosed untreated RA patients and HDs. We observed that the proportion of CD21+CD27+ MBCs correlated positively with RF and ACPA titers. In addition, the frequency of CD21+ DN cells and CD21-/low DN MBCs correlated positively with tender joint count and joint narrowing score respectively.
In conclusion, it seems that different MBCs have different roles in RA where CD21+ CD27+ MBCs appear to drive the autoantibody response, the CD21+DN MBCs the joint inflammation and the CD21-/low DN MBCs the joint damage.
Parts of work
I. Thorarinsdottir K*, Camponeschi A*, Cavallini N*, Grimsholm O, Jacobsson L, Gjertsson I, Mårtensson I-L. CD21-/low B cells in human blood are memory cells. Clin Exp Immunol. 2016; 185: 252-262.
*These authors contributed equally to the study ::pmid::27010233 II. Thorarinsdottir K, Camponeschi A, Jonsson C, Nilsson J, Forslind K, Visentini M, Jacobsson L, Mårtensson I-L, Gjertsson I. CD21-/low B cells associate with joint damage in rheumatoid arthritis patients.
Submitted III.Thorarinsdottir K, Forslind K, Agelii ML, Rudin A, Jacobsson L, Mårtensson I-L, Gjertsson I. Memory B cell subsets correlate with autoantibody titers, disease activity and joint damage in untreated early rheumatoid arthritis.
In Manuscript
Degree
Doctor of Philosophy (Medicine)
University
University of Gothenburg. Sahlgrenska Academy
Institution
Institute of Medicine. Department of Rheumatology and Inflammation Research
Disputation
Fredagen den 26 april 2019, kl. 9.00, Föreläsningssal våning 3, Guldhedsgatan 10A, Göteborg
Date of defence
2019-04-26
katrin.thorarinsdottir@vgregion.se
Date
2019-04-04Author
Thorarinsdottir, Katrin
Keywords
B cells
Rheumatoid arthritis
Joint destruction
DAS28
CD21-/low B cells
Publication type
Doctoral thesis
ISBN
978-91-7833-351-6 (PDF)
978-91-7833-350-9 (PRINT)
Language
eng