Journal
ARTHRITIS & RHEUMATOLOGY
Volume 66, Issue 12, Pages 3371-3381Publisher
WILEY-BLACKWELL
DOI: 10.1002/art.38860
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Funding
- CODI program through University of Antioquia Medical Research Institute
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Objective. In various chronic inflammatory processes, both the proportion and numbers of monocyte subsets are altered. In systemic lupus erythematosus (SLE), this has not been clearly determined. The monocyte subpopulations in patients with SLE, patients with other autoimmune diseases, and healthy controls were evaluated. The effects of nonclassic monocytes and apoptotic cells (ACs) on the differentiation and function of CD14 CD16 monocytes were also studied. Methods. Monocyte subpopulations derived from the blood samples of SLE patients (n 88), patients with other autoimmune diseases (n 37), and healthy control subjects (n 61) were separated by fluorescence-activated cell sorting. To evaluate the effect of CD14 CD16 monocytes and ACs on the differentiation of CD14 CD16 monocytes, we developed a coculture model of highly purified sorted monocyte subpopulations, which were reconstituted with defined proportions of CD14 CD16 and CD14 CD16 monocytes in the presence or absence of ACs. After differentiation into macrophages, CD3 lymphocytes were added, and the proliferating cells and CD3 IFN cells were evaluated. A cytokine bead array panel was used to test the coculture supernatants. Results. There was a reduction in CD14 CD16 monocytes in patients with active SLE. Monocytes from SLE patients had decreased expression of HLA-DR and decreased ability to bind and phagocytize ACs. In healthy controls, but not SLE patients, treatment with macrophages derived from CD14 CD16 monocytes reduced T cell proliferation and proliferating CD3 IFN cells and increased the accumulation of tumor necrosis factor , interleukin-10 (IL-10), and IL-1 . Conclusion. Our findings show that CD14 CD16 monocytes, a population that is reduced and nonfunctional in SLE patients, have modulatory effects on CD14 CD16 monocytes and T cells.
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