The Tee family kinases are critical downstream regulators of antigen receptor signals in lymphocytes. As kinases, they act on critical substrates to regulate signals such as calcium increase leading to activation of transcription factors such as NFAT, NF kappa B and SRF. We now show here that ITK, a member of the Tee family of tyrosine kinases, has a kinase independent function. Mutants of ITK that lack kinase activity or a kinase domain can rescue cells lacking Tec family kinases for antigen receptor induced SRF activation, but not for NFAT, AP-1 or NF kappa B activation. Furthermore, expression of these mutants in WT cells enhanced SRF activation. This kinase independent function required the SH2 domain since a mutant lacking both the kinase and SH2 domains was much less effective at rescuing SRF activation. This kinase-deleted mutant could partially rescue ERK activation, and interact with multiple tyrosine phosphorylated proteins during antigen receptor signaling, suggesting that ITK uses a scaffolding function that regulates signals leading to specific regulation of SRF activation. (c) 2006 Federation of European Biochemical Societies. Published by Elsevier B.V. All rights reserved.
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DNAX Res. Inst. Molec./Cell. Biology, Palo Alto
Howard Hughes Medical Institute, Univ. of California at San Francisco, San Francisco, CA 94143, Third and Parnassus Ave.DNAX Res. Inst. Molec./Cell. Biology, Palo Alto
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DNAX Res. Inst. Molec./Cell. Biology, Palo Alto
Cancer Research Institute, UCSF, Mt. Zion Cancer Center, San Francisco, CA 94115DNAX Res. Inst. Molec./Cell. Biology, Palo Alto
McMahon M.
Wahl M.I.
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Howard Hughes Medical Institute, Dept. Microbiol. Immunol./Molec. Gen, Univ. of California at Los Angeles, Los AngelesDNAX Res. Inst. Molec./Cell. Biology, Palo Alto
Wahl M.I.
Witte O.N.
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Howard Hughes Medical Institute, Dept. Microbiol. Immunol./Molec. Gen, Univ. of California at Los Angeles, Los AngelesDNAX Res. Inst. Molec./Cell. Biology, Palo Alto
Witte O.N.
Kurosaki T.
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Department of Molecular Genetics, Kansai Medical University, Moriguchi 570DNAX Res. Inst. Molec./Cell. Biology, Palo Alto
Kurosaki T.
Bolen J.B.
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DNAX Res. Inst. Molec./Cell. Biology, Palo Alto
Cancer Research Institute, UCSF, Mt. Zion Cancer Center, San Francisco, CA 94115DNAX Res. Inst. Molec./Cell. Biology, Palo Alto
Bolen J.B.
Johnston J.A.
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DNAX Res. Inst. Molec./Cell. Biology, Palo Alto
Department of Immunology, Queen's University Belfast, Belfast BT9 7BLDNAX Res. Inst. Molec./Cell. Biology, Palo Alto
机构:
DNAX Res. Inst. Molec./Cell. Biology, Palo Alto
Howard Hughes Medical Institute, Univ. of California at San Francisco, San Francisco, CA 94143, Third and Parnassus Ave.DNAX Res. Inst. Molec./Cell. Biology, Palo Alto
机构:
DNAX Res. Inst. Molec./Cell. Biology, Palo Alto
Cancer Research Institute, UCSF, Mt. Zion Cancer Center, San Francisco, CA 94115DNAX Res. Inst. Molec./Cell. Biology, Palo Alto
McMahon M.
Wahl M.I.
论文数: 0引用数: 0
h-index: 0
机构:
Howard Hughes Medical Institute, Dept. Microbiol. Immunol./Molec. Gen, Univ. of California at Los Angeles, Los AngelesDNAX Res. Inst. Molec./Cell. Biology, Palo Alto
Wahl M.I.
Witte O.N.
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h-index: 0
机构:
Howard Hughes Medical Institute, Dept. Microbiol. Immunol./Molec. Gen, Univ. of California at Los Angeles, Los AngelesDNAX Res. Inst. Molec./Cell. Biology, Palo Alto
Witte O.N.
Kurosaki T.
论文数: 0引用数: 0
h-index: 0
机构:
Department of Molecular Genetics, Kansai Medical University, Moriguchi 570DNAX Res. Inst. Molec./Cell. Biology, Palo Alto
Kurosaki T.
Bolen J.B.
论文数: 0引用数: 0
h-index: 0
机构:
DNAX Res. Inst. Molec./Cell. Biology, Palo Alto
Cancer Research Institute, UCSF, Mt. Zion Cancer Center, San Francisco, CA 94115DNAX Res. Inst. Molec./Cell. Biology, Palo Alto
Bolen J.B.
Johnston J.A.
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机构:
DNAX Res. Inst. Molec./Cell. Biology, Palo Alto
Department of Immunology, Queen's University Belfast, Belfast BT9 7BLDNAX Res. Inst. Molec./Cell. Biology, Palo Alto