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The Related Adhesion Focal Tyrosine Kinase Differentially Phosphorylates p130Cas and the Cas-like Protein, p105HEF1
Astier, Anne ; Manié, Serge N. ; Avraham, Hava ; Hirai, Hisamaru ; Law, Susan F. ; Zhang, Yuzhu ; ; Fu, Yigong ; Druker, Brian J. ; Haghayeghi, Nilou ... show 2 more
Astier, Anne
Manié, Serge N.
Avraham, Hava
Hirai, Hisamaru
Law, Susan F.
Zhang, Yuzhu
Fu, Yigong
Druker, Brian J.
Haghayeghi, Nilou
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Journal article
Date
1997-08-08
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Cancer and Cellular Biology
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https://doi.org/10.1074/jbc.272.32.19719
Abstract
The related adhesion focal tyrosine kinase (RAFTK) is tyrosine-phosphorylated following β1 integrin or B cell antigen receptor stimulation in human B cells. Two substrates that are tyrosine-phosphorylated following integrin ligation in B cells are p130Cas and the Cas family member human enhancer of filamentation 1 (HEF1), both of which can associate with RAFTK. In this report we observed that RAFTK was involved in the phosphorylation of these two proteins. While a catalytically active RAFTK was required for both p130Cas and HEF1, phosphorylation of p130Cas, but not of HEF1, was dependent on an intact autophosphorylation site (Tyr402) on RAFTK. To determine if RAFTK phosphorylated p130Cas and HEF1 directly or through an intermediate, we assayed the ability of RAFTK and of a Tyr402 mutant to phosphorylate purified HEF1 and p130Cas domains. RAFTK was able to phosphorylate the substrate domains of both p130Cas and HEF1, but only the C-terminal domain of p130Cas. Furthermore, Tyr402, which mediates the binding of RAFTK to c-Src kinase, was required for the phosphorylation of the C-terminal domain of p130Cas. These data suggest that RAFTK itself is sufficient for HEF1 phosphorylation, whereas a cooperation between RAFTK and Src kinases is required for the complete phosphorylation of p130Cas.
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Citation
Astier A, Manié SN, Avraham H, Hirai H, Law SF, Zhang Y, et al. The Related Adhesion Focal Tyrosine Kinase Differentially Phosphorylates p130Cas and the Cas-like Protein, p105HEF1. J Biol Chem. 1997 Aug 8;272(32):19719-19724. doi:10.1074/jbc.272.32.19719.
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Elsevier
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Journal of Biological Chemistry, Vol. 272, Iss. 32
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