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Literature DB >> 11860343

Recognition of multiple substrate motifs by the c-ABL protein tyrosine kinase.

Jinzi J Wu¹, Daniel E H Afar, Hoang Phan, Owen N Witte, Kit S Lam.

Abstract

Using a combinatorial peptide library that is based on the one-bead one-peptide approach we identified 14 peptide substrates for the c-ABL protein tyrosine kinase, which define three distinct consensus sequence groups. This is distinct from many serine/threonine kinases, which often phosphorylate only one major consensus sequence. The three consensus sequences accurately predict phosphorylation sites in cellular ABL substrates proven to play a role in cell signaling. Our data suggest that protein tyrosine kinases have evolved to recognize multiple substrate motifs.

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Year: 2002 PMID： 11860343 DOI： 10.2174/1386207023330516

Source DB: PubMed Journal: Comb Chem High Throughput Screen ISSN： 1386-2073 Impact factor: 1.339

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Recognition of multiple substrate motifs by the c-ABL protein tyrosine kinase.

1. Metabolism of peptide reporters in cell lysates and single cells.

2. Screening of a one bead-one compound combinatorial library for beta-actin identifies molecules active toward Ramos B-lymphoma cells.

3. Kinase-Catalyzed Biotinylation.

4. Chemoenzymatic Semi-synthesis Enables Efficient Production of Isotopically Labeled α-Synuclein with Site-Specific Tyrosine Phosphorylation.

5. Differential modification of p27Kip1 controls its cyclin D-cdk4 inhibitory activity.

6. RNA interference screen identifies Abl kinase and PDGFR signaling in Chlamydia trachomatis entry.

7. Protein and Chemical Microarrays-Powerful Tools for Proteomics.