Signal transduction mechanisms involved in mouse embryonic liver formation

2001 Fiscal Year Final Research Report Summary

• Project/Area Number: 12470493
• Research Category: Grant-in-Aid for Scientific Research (B)
• Allocation Type: Single-year Grants
• Section: 一般
• Research Field: Biological pharmacy
• Research Institution: The University of Tokyo
• Principal Investigator: NISHINA Hiroshi The University of Tokyo, Graduate School of Pharmaceutical Sciences, Dept. of Physiol. Chem., Associate Professor, 大学院・薬学研究科, 助教授 (60212122)
• Co-Investigator(Kenkyū-buntansha): KONTANI Kenji The University of Tokyo, Graduate Schdor of Pharmaceutical Sciences, Dept. of Physiol. Chem., Research fellow, 大学院・薬学研究科, 助手 (30302615) ; HOSHINO Shin-ichi The University of Tokyo, Graduate Schdor of Pharmaceutical Sciences, Dept. of Physiol. Chem., Lecturer, 大学院・薬学研究科, 講師 (40219168) ; TAKADA Toshiaki The University of Tokyo, Graduate School of Pharmaceutical Sciences, Dept. of Physiol. Chem., Professor, 大学院・薬学研究科, 教授 (10088859)
• Project Period (FY): 2000 – 2001
• Keywords: fetal liver / hepatic bud / MAP kinase / SEK1 / JNK / c-Jun / hematopoietic stem cells / NFκB

Research Abstract

Mice lacking stress-signaling kinase SEK1 die from embryonic day 10.5 (E10.5) to E12.5. Although a defect in liver formation is accompanied with the embryonic lethality of sek1-/- mice, the mechanism leading to the liver defect has remained unknown. Here we investigated liver development in sek1-/- embryos using a monoclonal antibody specifically recognizing murine hepatoblasts and genetic interaction of sek1 with proto-oncogene c-jun and tumor necrosis factor-α receptor 1 gene, tnfr1, which are also responsible for liver formation and the cell apoptosis. There was a progressive increase in the hepatoblast cell numbers of wild-type embryos from E10.5 to 12.5. The hepatoblast proliferation required no hematopoiesis, since transcription factor AML1-deficient mice had no defect in the cell growth. Instead, impaired hepatoblast proliferation was observed in sek1-/- livers from E10.5, though fetal liver-specific gene expression was normal. The impaired phenotype in sek1-/- livers was more severe than in c-jun-/- embryos, and sek1-/- c-jun-/- embryos more rapidly died before E8.5. Stimulation of stress-activatied protein kinase/c-Jun N-terminal kinase by hepatocyte growth factor was attenuated in sek1-/- livers. The defective liver formation in sek1-/- embryos was not protected by additional tnfr1 mutation that rescues the embryonic lethality of mice lacking NF-κB signaling components. Thus, SEK1 appears to play a crucial role in hepatoblast proliferation and survival in a manner apparently different from c-Jun or NF-κB.

Research Products

• [Publications] K.Bachmaier, C.Krawczyk, I.Kozieradzki, et al.: "Negative regulation of lymphocyte activation and autoimmunity by the molecular adaptor Cbl-b"Nature. 403. 211-216 (2001)
  • Description: 「研究成果報告書概要(和文)」より
• [Publications] T.Wada, K.Nakagawa, G.Nishitai, et al.: "Impaired synergistic activation of stress-activated protein kinase SAPK/JNK in ES cells lacking SEK1/MKK4"J. Biol. Chem.. 276. 30892-30897 (2001)
  • Description: 「研究成果報告書概要(和文)」より
• [Publications] T.Sasaki, T.Wada, H.Kishimoto, et al.: "he stress kinase MKK7 is a negative regulator of antigen receptor and growth factor receptor induced proliferation in hematopoietic cells"J. Exp. Med.. 17. 757-768 (2001)
  • Description: 「研究成果報告書概要(和文)」より
• [Publications] H.Yoshida, S.Hamano, G.Senaldi, et al.: "WSX-1 is required for the initiation of Th1 responses and resistance to L. major infection"Immunity. 15. 569-578 (2001)
  • Description: 「研究成果報告書概要(和文)」より
• [Publications] D.Kitagawa, S.Tanemura, S.Ohata, et al.: "Activation of extracellular signal-regulated kinase by ultraviolet is mediated through Src-dependent epidermal growth factor receptor phosphorylation"J. Biol. Chem.. 276. 366-371 (2002)
  • Description: 「研究成果報告書概要(和文)」より
• [Publications] K. Bachmaier, C. Krawczyk, I. Kozieradzki, Y-Y. Kong, T. Sasaki, A. Oliveira-dos-Santos, S. Mariathasan, D. Bouchard, A. Wakeham, A. Itie, J. Le, P. Ohashi, I. Sarosi, H. Nishina, S. Lipkowitz, & J.M. Penninger: "Negative regulation of lymphocyte activation and autoimmunity by the molecular adaptor Cbl-b"Nature. 403. 211-216 (2000)
  • Description: 「研究成果報告書概要(欧文)」より
• [Publications] T. Wada, K. Nakagawa, G. Nishitai, J. Seo, H. Kishimoto, T. Watanabe, D. Kitagawa, T. Sasaki, J. M. Penninger, H. Nishina, & T Katada: "Impaired synergistic activation of stress-activated protein kinase SAPK/JNK in ES cells lacking SEK1/MKK4"J. Biol. Chem.. 276. 30892-30897 (2001)
  • Description: 「研究成果報告書概要(欧文)」より
• [Publications] T. Sasaki, T, Wada, H, Kishimoto, J. Irie-Sasaki, G. Matsumoto, T. Goto, Z, Yao, A. Wakeham, T. W. Mak, A. Suzuki, T. Katada, H. Nishina, & J. M. Penninger: "The stress kinase MKK7 is a negative regulator of antigen receptor and growth factor receptor induced proliferation in hematopoietic cells"J. Exp. Med.. 17. 757-768 (2001)
  • Description: 「研究成果報告書概要(欧文)」より
• [Publications] H. Yoshida, S. Hamano, G. Senaldi, T. Covey, R. Faggioni, S. Mu, M. Xia, A. Wakeham, H. Nishina, J. Potter, C. J. M. Saris, & T. W. Mak: "WSX-1 is required for the initiation of Th1 responses and resistance to L. major infection"Immunity. 15. 569-578 (2001)
  • Description: 「研究成果報告書概要(欧文)」より
• [Publications] D. Kitagawa, S. Tanemura, S. Ohata, N. Shimizu, J. Seo, G. Nishitai, T. Watanabe, K. Nakagawa, H. Kishimoto, T, Wada, T. Tezuka, T. Yamamoto, H. Nishina, & T. Katada T: "Activation of extracellular signal-regulated kinase by ultraviolet is mediated through src-dependent epidermal growth factor receptor phosphorylation : Its implication in an anti-apoptotic function"J. Biol. Chem.. 277. 366-371 (2002)
  • Description: 「研究成果報告書概要(欧文)」より