ACR Meeting Abstracts

ACR Meeting Abstracts

Abstract Number: 1828

Metabolic Reprogramming in CD4+CD28-CXCR3intt-bethi cells and Its Relevance to Pathogenesis in Patients with SLE

Shigeru Iwata1, Yuka Kanno2, Kei Sakata3,4, Maiko Hajime1, Masataka Torigoe1,5, Naoaki Ohkubo1, Shingo Nakayamada6, John J O'Shea7 and Yoshiya Tanaka8, 1The First Department of Internal Medicine, University of Occupational and Environmental Health, Japan, Kitakyushu, Japan, 2National Institute of Arthritis and Musculoskeletal and Skin Diseases, NIH, Bethesda, MD, 3Mitsubishi Tanabe Pharma Corporation, Tokyo, Japan, 4The First Department of Internal Medicine, University of Occupational and Environmental Health, Japan, Kitakyshu, Japan, 5Department of Endocrinology, Metabolism, Rheumatology and Nephrology,, Faculty of Medicine, Oita University, Yufu, Oita, Japan, Yufu, Japan, 6First Department of Internal Medicine, University of Occupational and Environmental Health, Japan, Kitakyushu, Japan, 7NIAMS NIH, National Institute of Arthritis and Musculoskeletal and Skin Diseases, NIH, Bethesda, MD, 8University of Occupational and Environmental Health, Kitakyushu, Japan

Meeting: 2016 ACR/ARHP Annual Meeting

Date of first publication: September 28, 2016

Keywords: ,

Session Information

Date: Monday, November 14, 2016

Title: Systemic Lupus Erythematosus – Human Etiology and Pathogenesis - Poster I

Session Type: ACR Poster Session B

Session Time: 9:00AM-11:00AM

Background/Purpose: CD4+ T cells play a crucial role in pathological process of Systemic Lupus Erythematosus (SLE). Recently, importance of metabolic reprograming in immunocompetent cells was highlighted. We found that preferential induction of T-bet by IFN-γ is an important factor for shift to glycolysis in activated CD4+ T cells in vitro. In this study, we examine the mechanism by which IFN-γ and T-bet in CD4+T cells involved in pathogenesis of SLE.

Methods: Peripheral blood mononuclear cells were obtained from 19 healthy controls (HCs), 30 patients with bio-naïve active RA and 60 patients with active SLE. The expression of CXCR3, T-bet, mTORC1 phosphorylation and IFN-γ production in CD4+T cells were measured by flow cytometry, and assessed the correlation with clinical characteristics.

Results: We found that CD4+ T cells consisted of 3 subsets of CD28+CXCR3lo T-betlo cells (R1), CD28+CXCR3hiT-betint cells (R2), CD28CXCR3intT-bethi cells (R3). The percentage of R3 in SLE patients was significantly higher compared to HCs (HCs; 1.1±0.2%, RA; 5.5±1.8%, p=0.06, SLE; 5.6±1.1%, p=0.02). CD4+CD28CXCR3intT-bethi cells mainly consisted of CD45RACCR7 effector memory cells and were significantly activated compared to other subsets (HLA-DR+CD38+ cells; R1: 2.8±0.6%, R2: 11.2±1.5%, R3: 27.6±2.3%, p<0.0001, ANOVA). CD4+CD28CXCR3intT-bethi cells from SLE patients showed pronounced IFN-γ production compared to HCs (T-bethi IFN-γ+ cells; HCs: 1.1±0.4%, RA: 1.7±0.6%, p=0.50, SLE: 5.6±1.3%, p=0.04). Interestingly, the ratio of CD4+CD28CXCR3intT-bethi cells was significantly correlated with the number of immunosuppressants previously used for the SLE patients, that is treatment-resistant (p=0.03, logistic regression analysis). Phosphorylation of mTORC1, which is important for shift to glycolysis, in CD4+ T cells from patients with RA and SLE was significantly increased compared to HCs (ΔMFI of p-mTORC1; HCs: 284.9, RA: 563, p=0.01, SLE: 511.7, p=0.03). T-bet expression was significantly correlated with mTOC1 phosphorylation and IFN-γ production in CD4+T cells from patients with SLE (p-mTORC1: r=0.4718, p<0.01, IFN-γ production: r=0.4915, p=0.01, Pearson).

Conclusion: These results indicated that CD4+CD28CXCR3intT-bethi cells might be related to refractory to established therapies in patients with SLE. In addition, these cells are constitutively activated accompanied with shift to glycolysis through IFN-γ-mTORC1-T-bet pathway. We highlight CD4+CD28CXCR3intT-bethi cells and their metabolic reprogramming as a potential target for pathological process in SLE.

Disclosure: S. Iwata, None; Y. Kanno, None; K. Sakata, N/A, 3; M. Hajime, None; M. Torigoe, None; N. Ohkubo, None; S. Nakayamada, None; J. J. O'Shea, None; Y. Tanaka, N/A, 5.

To cite this abstract in AMA style:

Iwata S, Kanno Y, Sakata K, Hajime M, Torigoe M, Ohkubo N, Nakayamada S, O'Shea JJ, Tanaka Y. Metabolic Reprogramming in CD4+CD28-CXCR3intt-bethi cells and Its Relevance to Pathogenesis in Patients with SLE [abstract]. Arthritis Rheumatol. 2016; 68 (suppl 10). https://acrabstracts.org/abstract/metabolic-reprogramming-in-cd4cd28-cxcr3intt-bethi-cells-and-its-relevance-to-pathogenesis-in-patients-with-sle/. Accessed .

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