Myeloid deletion of SIRT1 suppresses collagen-induced arthritis in mice by modulating dendritic cell maturation

The type III histone deacetylase silent information regulator 1 (SIRT1) is an enzyme that is critical for the modulation of immune and inflammatory responses. However, the data on its role in rheumatoid arthritis (RA) are limited and controversial. To better understand how SIRT1 regulates adaptive i...

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Bibliographic Details
Published in:Experimental & molecular medicine 2016-03, Vol.48 (3), p.e221-e221
Main Authors: Woo, Seong Ji, Lee, Sang-Myeong, Lim, Hye Song, Hah, Young-Sool, Jung, In Duk, Park, Yeong-Min, Kim, Hyun-Ok, Cheon, Yun-Hong, Jeon, Min-Gyu, Jang, Kyu Yun, Kim, Kyeong Min, Park, Byung-Hyun, Lee, Sang-Il
Format: Article
Language:English
Subjects:
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Animals
Arthritis, Experimental - diagnosis
Arthritis, Experimental - etiology
Arthritis, Experimental - metabolism
Biomedical and Life Sciences
Biomedicine
Cell Differentiation
Coculture Techniques
Cytokines - genetics
Cytokines - metabolism
Dendritic Cells - cytology
Dendritic Cells - immunology
Dendritic Cells - metabolism
Disease Models, Animal
Gene Deletion
Gene Expression Regulation
Humans
Inflammation Mediators - metabolism
Lymph Nodes - immunology
Lymph Nodes - metabolism
Medical Biochemistry
Mice
Mice, Knockout
Molecular Medicine
Myeloid Cells - metabolism
NF-kappa B - metabolism
Original
original-article
Sirtuin 1 - genetics
Stem Cells
Synovitis - genetics
Synovitis - immunology
Synovitis - metabolism
Synovitis - pathology
Th1 Cells - cytology
Th1 Cells - immunology
Th1 Cells - metabolism
Th17 Cells - cytology
Th17 Cells - immunology
Th17 Cells - metabolism
Transcription Factor AP-1 - metabolism
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Summary:The type III histone deacetylase silent information regulator 1 (SIRT1) is an enzyme that is critical for the modulation of immune and inflammatory responses. However, the data on its role in rheumatoid arthritis (RA) are limited and controversial. To better understand how SIRT1 regulates adaptive immune responses in RA, we evaluated collagen-induced arthritis (CIA) in myeloid cell-specific SIRT1 knockout (mSIRT1 KO) and wild-type (WT) mice. Arthritis severity was gauged on the basis of clinical, radiographic and pathologic scores. Compared with their WT counterparts, the mSIRT1 KO mice exhibited less severe arthritis, which was less destructive to the joints. The expression levels of inflammatory cytokines, matrix metalloproteinases and ROR-γT were also reduced in the mSIRT1 KO mice compared with the WT mice and were paralleled by reductions in the numbers of Th1 and Th17 cells and CD80- or CD86-positive dendritic cells (DCs). In addition, impaired DC maturation and decreases in the Th1/Th17 immune response were observed in the mSIRT1 KO mice. T-cell proliferation was also investigated in co-cultures with antigen-pulsed DCs. In the co-cultures, the DCs from the mSIRT1 KO mice showed decreases in T-cell proliferation and the Th1/Th17 immune response. In this study, myeloid cell-specific deletion of SIRT1 appeared to suppress CIA by modulating DC maturation. Thus, a careful investigation of DC-specific SIRT1 downregulation is needed to gauge the therapeutic utility of agents targeting SIRT1 in RA. Rheumatoid arthritis: Mice protected from disease when deficient for enzyme Mice lacking a key immune-regulating enzyme are less prone to develop rheumatoid arthritis. A research team led by Sang-Il Lee from the Gyeongsang National University School of Medicine in South Korea evaluated the immune response of mice with experimentally induced rheumatoid arthritis. The researchers looked both in normal mice and those genetically engineered not to produce SIRT1, an enzyme known to regulate aging, cellular stress responses, metabolism and inflammation. The myeloid-specific SIRT1 conditional knockout mice had less severe disease, owing to reduced levels of several immune molecules. In ex-vivo and in vitro , the researchers showed that one type of immune cell, called a dendritic cell, was less likely to mature and drive less inflammatory response when taken from SIRT1-deficient mice. The findings suggest that targeting SIRT1 with drugs could help in the clinical manageme
ISSN:2092-6413
1226-3613
2092-6413
DOI:10.1038/emm.2015.124