Expansion of PD-1-Positive Effector CD4 T Cells in an Experimental Model of SLE: Contribution to the Self-Organized Criticality Theory
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概要
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We have developed a systems biology concept to explain the origin of systemic autoimmunity. From our studies of systemic lupus erythematosus (SLE) we have concluded that this disease is the inevitable consequence of over-stimulating the host's immune system by repeated exposure to antigen to levels that surpass a critical threshold, which we term the system's "self-organized criticality". We observed that overstimulation of CD4 T cells in mice led to the development of autoantibody-inducing CD4 T cells (aiCD4 T) capable of generating various autoantibodies and pathological lesions identical to those observed in SLE. We show here that this is accompanied by the significant expansion of a novel population of effector T cells characterized by expression of programmed death-1 (PD-1)-positive, CD27low, CD127low, CCR7low and CD44highCD62Llow markers, as well as increased production of IL-2 and IL-6. In addition, repeated immunization caused the expansion of CD8 T cells into fully-matured cytotoxic T lymphocytes (CTL) that express Ly6ChighCD122high effector and memory markers. Thus, overstimulation with antigen leads to the expansion of a novel effector CD4 T cell population that expresses an unusual memory marker, PD-1, and that may contribute to the pathogenesis of SLE.
- 2013-00-00
著者
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Shiozawa Shunichi
Department Of Gastroenterology And Hepatology Shimane University School Of Medicine
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Ito Mitsuhiro
Department Of Anesthesiology Kanagawa Dental College
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Tsumiyama Ken
Department Of Biophysics Kobe University Graduate School Of Health Sciences
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YAMANE Takashi
Rheumatic Disease Center, Konan Kakogawa Hospital
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Shiozawa Shunichi
Department of Medicine, Kyushu University Beppu Hospital
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Tsumiyama Ken
Department of Medicine, Kyushu University Beppu Hospital
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Miyazaki Yumi
Department of Biophysics, Kobe University Graduate School of Health Science
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