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Over-expression of Roquin aggravates T cell mediated hepatitis in transgenic mice using T cell specific promoter
Authors:Young Rae Ji  Hei Jung Kim  Dong Hun Yu  Ki Beom Bae  Seo Jin Park  Si Jun Park  Woo Young Jang  Min-Cheol Kang  Jain Jeong  Yong Hun Sung  Minjee Choi  Taejun Park  Taesun Park  Jong Won Yun  Hyun-Shik Lee  Sanggyu Lee  Myoung Ok Kim  Zae Young Ryoo
Affiliation:1. School of Life Science, KNU Creative BioResearch Group (BK21 plus project), Kyungpook National University, Buk-ku, Daegu, Republic of Korea;2. Department of Biotechnology, Daegu University, Kyungsan, Kyungbuk, Republic of Korea;3. Department of Food and Nutrition, Brain Korea 21 PLUS Project, Yonsei University, 50 Yonsei-ro, Seodaemun-gu, Seoul, Republic of Korea;4. Departments of Animal Science, Kyungpook National University, Sangju, Republic of Korea
Abstract:Chronic hepatitis is a major cause of liver cancer, so earlier treatment of hepatitis might be reducing liver cancer incidence. Hepatitis can be induced in mice by treatment with Concanavalin A (Con A); the resulting liver injury causes significant CD4+ T cell activation and infiltration. In these T cells, Roquin, a ring-type E3 ubiquitin ligase, is activated. To investigate the role of Roquin, we examined Con A-induced liver injury and T cell infiltration in transgenic (Tg) mice overexpressing Roquin specifically in T cells. In Roquin Tg mice, Con A treatment caused greater increases in both the levels of liver injury enzymes and liver tissue apoptosis, as revealed by TUNEL and H&E staining, than wild type (WT) mice. Further, Roquin Tg mice respond to Con A treatment with greater increases in the T cell population, particularly Th17 cells, though Treg cell counts are lower. Roquin overexpression also enhances increases in pro-inflammatory cytokines, including IFN-γ, TNF-α and IL-6, upon liver injury. Furthermore, Roquin regulates the immune response and apoptosis in Con A induced hepatitis via STATs, Bax and Bcl2. These findings suggest that over-expression of Roquin exacerbates T-cell mediated hepatitis.
Keywords:Con A  concanavalin A  Tg  transgenic  TUNEL  terminal deoxynucleotidyl transferase mediated dUTP Nick End Labeling  H&  E  hematoxylin and eosin  WT  wild type  Th17  interleukin-17 secreting CD4 T helper cells  Treg  regulatory T helper cells  IFN-γ  interferon gamma  TNF-α  tumor necrosis factor-alpha  IL  interleukin  Bax  Bcl2 associated X  Bcl-2  B cell lymphoma 2  ICOS  inducible T cell co-stimulator  Tfh  follicular T helper cells  CIA  collagen induced arthritis  FACS  fluorescence activated cell sorter  ELISA  enzyme linked immunoassay
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