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2018 Fiscal Year Final Research Report

Elucidation of molecular mehcanisms of autoimmune pancreatitis

Research Project

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Project/Area Number 16K08740
Research Category

Grant-in-Aid for Scientific Research (C)

Allocation TypeMulti-year Fund
Section一般
Research Field Experimental pathology
Research InstitutionYamaguchi University (2018)
Kyushu University (2016-2017)

Principal Investigator

SHIBATA Kensuke  山口大学, 大学院医学系研究科, 講師 (50529972)

Research Collaborator YAMASAKI Sho  
OGAWA Yoshihiro  
Project Period (FY) 2016-04-01 – 2019-03-31
Keywords自己免疫疾患 / 代謝産物 / T細胞
Outline of Final Research Achievements

Autoimmune diseases are frequently caused by pathogenic T cells, but identities of the pathogenic T cell subsets remain unclear. Here we established a mouse model in which spontaneously develops a fatal autoimmune disease with severe pancreatic inflammation accompanied by autoantibody deposition and B cell infiltration. We found that MR1-restricted αβ T (MR1T) cells expanded in response to pancreas-derived autoantigens and genetic deletion of MR1T cells significantly prolonged their survival. The disease manifestations in mice recapitulated human autoimmune pancreatitis (AIP) and, frequency of activated MR1T cells was significantly enhanced in AIP patients. Thus, our study provides a novel insight into the mechanism of T cell-mediated autoimmune diseases.

Free Research Field

免疫学

Academic Significance and Societal Importance of the Research Achievements

本研究は、我々が独自に樹立したヒトIgG4関連疾患様病態自然発症マウスモデルを用いた臨床応用研究であり、極めて独創性が高く学術的意義は高い。また、ヒトIgG4関連疾患の病態を反映したバイオマーカーは未だ同定されておらず、今後の研究で我々が同定した病原性MR1T細胞のバイオマーカーとしての有効性が示されれば、世界初のIgG4関連疾患発症や再発を予測できる手法となることが期待され社会的ニーズも高いと考えられる。

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Published: 2020-03-30  

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