Abstract
Out of the 90 human protein tyrosine kinases, 81 were assayed with short peptides derived from wellcharacterized [CDK1(Tyr15), IRS1(Tyr983), and JAK1(Tyr1023)] or generic [polyGlu:Tyr(4:1) and polyGlu:Ala:Tyr(1:1:1)] substrates. As expected, the CDK1 peptide is a substrate for all Src family kinases. On the other hand, some of the activities are novel and lead to a better understanding of the function of certain kinases. Specifically, the CDK1 peptide is a substrate for many of the Eph family members. Interestingly, profiling of nearly all the human protein tyrosine kinases revealed a distinct pattern of selectivity towards the CDK1 and IRS1 peptides. © Blouin et al.
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Blouin, J., Roby, P., Arcand, M., Beaudet, L., & Lipari, F. (2011). Catalytic specificity of human protein tyrosine kinases revealed by peptide substrate profiling. Current Chemical Genomics, 5(1), 115–121. https://doi.org/10.2174/1875397301105010115
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