Add to ORKGA series of conformationally constrained peptides were designed and synthesized as the Src SH2 domain ligands based on a tetrapeptide sequence pTyr-Glu-Glu-Ile (pYEEI). In general, the constrained peptides such as compounds 6, 7, and 11 (IC50 = 1.1-1.5 μM) showed higher binding affinities to the Src SH2 domain relative to the corresponding linear peptides 8a, 9a, and 13a, respectively (IC50 \u3e 100 μM), and PYEEI (IC50 = 6.5 μM), as evaluated by a fluorescence polarization assay. Molecular modeling studies revealed that in constrained peptides, the isoleucine side chain penetrates very deeply into the hydrophobic binding pocket (P + 3 site) of the Src SH2 domain. These constrained peptides can serve as novel templates for the design of sma...
Src homology 2 (SH2) domains are found in a variety of signaling proteins and bind phosphotyrosine-c...
[[abstract]]One of the critical intracellular signal transduction pathways involves the binding of t...
A series of peptide analogues of Ac-CIYKYY (1) were synthesized by functional group modifications in...
Src kinase activity is regulated by the interaction of SH3 domain with protein sequences that are ri...
Src homology-2 (SH2) domains are noncatalytic motifs containing approximately 100 amino acid residue...
Src kinase activity is regulated by the interaction of SH3 domain with protein sequences that are ri...
The diversity of amino acids in peptides allows the design of different linear or cyclized compounds...
Phosphopeptide pTyr-Glu-Glu-Ile (pYEEI) has been introduced as an optimal Src SH2 domain ligand. Pep...
SummarySite-directed mutagenesis to the 20 natural amino acids becomes a limitation when evaluating ...
Site-directed mutagenesis to the 20 natural amino acids becomes a limitation when evaluating subtle ...
The crystal structure of the Src SH2 domain complexed with a high affinity 11-residue phosphopeptide...
Phosphopeptide pTyr-Glu-Glu-Ile (pYEEI) has been introduced as an optimal Src SH2 domain ligand. Pep...
segments by Src homology 2 (SH2) and phosphotyrosine-binding (PTB) domains plays an important role i...
SH2 domains provide fundamental recognition sites in tyrosine kinase-mediated signaling pathways whi...
Background: Specific recognition of phosphotyrosine-containing protein segments by Src homology 2 (S...
Src homology 2 (SH2) domains are found in a variety of signaling proteins and bind phosphotyrosine-c...
[[abstract]]One of the critical intracellular signal transduction pathways involves the binding of t...
A series of peptide analogues of Ac-CIYKYY (1) were synthesized by functional group modifications in...
Src kinase activity is regulated by the interaction of SH3 domain with protein sequences that are ri...
Src homology-2 (SH2) domains are noncatalytic motifs containing approximately 100 amino acid residue...
Src kinase activity is regulated by the interaction of SH3 domain with protein sequences that are ri...
The diversity of amino acids in peptides allows the design of different linear or cyclized compounds...
Phosphopeptide pTyr-Glu-Glu-Ile (pYEEI) has been introduced as an optimal Src SH2 domain ligand. Pep...
SummarySite-directed mutagenesis to the 20 natural amino acids becomes a limitation when evaluating ...
Site-directed mutagenesis to the 20 natural amino acids becomes a limitation when evaluating subtle ...
The crystal structure of the Src SH2 domain complexed with a high affinity 11-residue phosphopeptide...
Phosphopeptide pTyr-Glu-Glu-Ile (pYEEI) has been introduced as an optimal Src SH2 domain ligand. Pep...
segments by Src homology 2 (SH2) and phosphotyrosine-binding (PTB) domains plays an important role i...
SH2 domains provide fundamental recognition sites in tyrosine kinase-mediated signaling pathways whi...
Background: Specific recognition of phosphotyrosine-containing protein segments by Src homology 2 (S...
Src homology 2 (SH2) domains are found in a variety of signaling proteins and bind phosphotyrosine-c...
[[abstract]]One of the critical intracellular signal transduction pathways involves the binding of t...
A series of peptide analogues of Ac-CIYKYY (1) were synthesized by functional group modifications in...