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Expression patterns of CD28 and CTLA‐4 in early, chronic, and untreated rheumatoid arthritis

Mariel García‐Chagollán, I. Y. Ledezma-Lozano, Jorge Hernández‐Bello, Pedro Ernesto Sánchez‐Hernández, Sergio Gutiérrez‐Ureña, José Francisco Muñóz-Valle

2020Journal of Clinical Laboratory Analysis25 citationsDOIOpen Access PDF

Abstract

BACKGROUND: T-cell activation pathways have been proposed as trigger mechanisms in the pathogenesis of rheumatoid arthritis (RA). CD28 and CTLA-4 play major roles in regulating the stimulatory and inhibitory co-signals in T cells. OBJECTIVE: To analyze the association between soluble and surface expression of CD28 and CTLA-4 with the clinical parameters of RA patients. METHODS: A total of 35 RA patients classified as early RA (n = 14), chronic RA (n = 14), and untreated RA (n = 7), as well as 7 age- and sex-matched control subjects (CS) were included. Surface expression of CD28 and CTLA-4 on T cells was evaluated by flow cytometry. Soluble levels of CD28 (sCD28), CTLA-4 (sCTLA-4), and anti-CCP antibodies were measured by ELISA. RESULTS: A significant lower percentage of CD8 + T cells positive to CD28 (CS = 64.9% vs RA = 42.7%, P = .04), and diminished surface expression of CD28 (CS: MFI = 122.9 vs RA: MFI = 33.1, P = .006), were found in chronic RA patients compared to CS. Higher sCD28 were observed in early RA patients compared with chronic RA patients (P < .05). sCTLA-4 was found increased in untreated RA patients compared to early RA patients (P < .05). sCD28 concentration correlated with anti-CCP levels (rho = -0.12; P = .032). The soluble and surface expressions of CTLA-4 were not associated with RA clinical parameters. CONCLUSIONS: In RA, the percentage of CD8 + CD28+ T cells decreases and expresses fewer membrane CD28 than CS. sCD28 levels are lower in chronic RA and are associated negatively with anti-CCP levels. sCTLA 4 levels are lower in early RA patients than in untreated RA patients.

Topics & Concepts

CD28Rheumatoid arthritisCTLA-4MedicinePathogenesisFlow cytometryCD8Internal medicineArthritisT cellImmunologyEndocrinologyImmune systemRheumatoid Arthritis Research and TherapiesT-cell and B-cell ImmunologyCancer Immunotherapy and Biomarkers