Deep Immunophenotyping of Circulating T and B Cells in Relapsing Adult-Onset Still’s Disease-Reference-Cited by-同舟云学术

Deep Immunophenotyping of Circulating T and B Cells in Relapsing Adult-Onset Still’s Disease

Published:2024-02-01 Issue:2 Volume:46 Page:1177-1191
ISSN:1467-3045
Container-title:Current Issues in Molecular Biology
language:en
Short-container-title:CIMB

Author:

Myachikova Valentina¹²,Kudryavtsev Igor²³,Rubinstein Artem²³^ORCID,Aquino Arthur²^ORCID,Isakov Dmitry⁴,Golovkin Alexey²^ORCID,Maslyanskiy Alexey¹⁵

Affiliation:

1. Rheumatology and Immunopathology Research Laboratory, Federal State Budgetary Institution “Almazov National Medical Research Centre” of the Ministry of Health of the Russian Federation, 197341 St. Petersburg, Russia

2. Autoimmune and Autoinflammatory Diseases Research Laboratory, Federal State Budgetary Institution “Almazov National Medical Research Centre” of the Ministry of Health of the Russian Federation, 197341 St. Petersburg, Russia

3. Laboratory of Cellular Immunology, Institute of Experimental Medicine, 197376 St. Petersburg, Russia

4. Department of Immunology, First St. Petersburg State Medical University, 197022 St. Petersburg, Russia

5. Scientific, Clinical and Educational Centre of Gastroenterology and Hepatology, Saint Petersburg State University, 199034 St. Petersburg, Russia

Abstract

Adult-onset Still’s disease (AOSD) is a complex systemic inflammatory disorder, categorized as an ‘IL-1 driven’ inflammasomapathy. Despite this, the interaction between T and B cells remains poorly understood. We conducted a study, enrolling 7 patients with relapsing AOSD and 15 healthy control subjects, utilizing deep flow cytometry analysis to examine peripheral blood T- and B-cell subsets. T-cell and B-cell subsets were significantly altered in patients with AOSD. Within CD4+ T cells, Th2 cells were decreased. Additionally, Th17 cell and follicular Th cell subsets were altered within CD45RA–CD62L+ and CD45RA–CD62L– Th cells in patients with AOSD compared to healthy controls. We identified changes in CD8+ T cell maturation and ‘polarization’ in AOSD patients, with an elevated presence of the TEMRA CD8+ T cell subset. Furthermore, the percentage of Tc1 cells was decreased, while the frequency of CCR6–CXCR3– Tc2 cells was elevated. Finally, we determined that the frequency of CD5+CD27– B cells was dramatically decreased in patients with AOSD compared to healthy controls. Further investigations on a large group of patients with AOSD are required to evaluate these adaptive immunity cells in the disease pathogenesis.

Funder

Ministry of Science and Higher Education of the Russian Federation

Publisher

MDPI AG

Subject

Microbiology (medical),Molecular Biology,General Medicine,Microbiology

Link

https://www.mdpi.com/1467-3045/46/2/75/pdf

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