Evidence of Autophosphorylation in Txk : Y91 Is an Autophosphorylation Site
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概要
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We have previously shown that Txk, a member of Tec family tyrosine kinase, is expressed in Th1 and Th0 cells and directly contributes to gene transcription of Th1-related proteins, including interferon (IFN)-γ, through nuclear translocation in response to mitogenic stimuli. Btk, another member of Tec family tyrosine kinase, has been shown to have a Src family tyrosine kinase-dependent transphosphorylation site and an autophosphorylation site. However, little is known about the phosphorylation mechanism of Txk, except that 420 tyrosine residue was identified as the trausphosphorylation site. In this study, we found that Txk autophosphorylated itself by using an in vitro kinase assay. To elucidate the role of phosphorylation in Txk function, we studied IFN-γ secretion by Jurkat T cells expressing mutant Txk proteins. While transfection with the wild,type Txk resulted in increased IFN-γ production, the function was abrogated by disruption of the ATP biding site, which is presumably involved in the autophosphorylation mechanism. The results suggest that phosphorylated Txk is an active form to promote IFN-γ synthesis. The 91 tyrosine residue of Txk is deduced to be an autophosphorylation site by comparing its structure with Btk. In Jurkat cells transfected with Txk Y91A, IFN-γ production was decreased in comparison with the wild-type Txk transfected Jurkat cells. These data suggest that phosphorylation of the 91 tyrosine residue in Txk plays a positive regulatory role in Txk function.
- 公益社団法人日本薬学会の論文
- 2002-06-01
著者
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Suzuki Noboru
Department of Advanced Interdisciplinary Sciences, Graduate School of Engineering, Utsunomiya Univer
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TAKENO Mitsuhiro
Department of Internal Medicine and Clinical Immunology, Yokohama City University Graduate School of
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Kashiwakura Jun-ichi
Department of Biochemistry, Hoshi University
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Nakajin Shizuo
Department of Biochemistry, Hoshi University School of Pharmacy and Pharmaceutical Sciences
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Takeno Mitsuhiro
Department Of Internal Medicine And Clinical Immunology Yokohama City University Graduate School Of
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Takeno Mitsuhiro
Departments Of Immunology And Medicine St.marianna University School Of Medicine
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ITOH Saotomo
Research Institute of Tuberculosis, Japan Anti-Tuberculosis Association
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OKU Teruaki
Department of Biochemistry, Hoshi University
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SAKANE Tsuyoshi
Departments of Immunology and Medicine, St.Marianna University School of Medicine
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TOYOSHIMA Satoshi
Pharmaceuticals and Medical Devices Evaluation Center National Institute of Health Sciences
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Oku Teruaki
Department Of Microbiology Hoshi University School Of Pharmacy And Pharmaceutical Sciences
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Oku Teruaki
Department Of Microbiology School Of Pharmacy Hoshi University
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NAKAJIN Shizuo
Hoshi University School of Pharmacy and Pharmaceutical Sciences
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Kashiwakura Jun-ichi
Department Of Biochemistry Hoshi University
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Toyoshima S
Department Of Biochemistry Faculty Of Pharmaceutical Sciences Hoshi University
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Toyoshima S
Pharmaceuticals And Medical Devices Agency
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Toyoshima Satoshi
Pharmaceutical And Medical Devices Evaluation Center National Institute Of Health Science
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Suzuki N
Laboratory Of Pharmacotherapeutics Department Of Pharmaceutical Sciences Josai International Univers
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Nozaki Seishiro
Department Of Pharmaceutical Sciences Tohoku University Hospital And Division Of Clinical Pharmacy G
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Oku T
Amagasaki Chemical Industries Co.
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Nakajin S
Hoshi University School Of Pharmacy And Pharmaceutical Sciences
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Nakajin Shizuo
Department Of Biochemistry Faculty Of Pharmaceutical Sciences Hoshi University
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Kashiwakura J
Department Of Biochemistry Hoshi University
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Itoh Saotomo
Department Of Microbiology Hoshi University School Of Pharmacy And Pharmaceutical Sciences
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Sakane T
St. Marianna Univ. School Of Medicine Kanagawa Jpn
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Sakane Tsuyoshi
Departments Of Immunology And Medicine St Marianna University School Of Medicine
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Suzuki Noboru
Department Of Advanced Interdisciplinary Sciences Graduate School Of Engineering Utsunomiya Universi
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