PDBsum entry 3f6x

Transferase

PDB id: 3f6x

Contents

Protein chains

264 a.a. *

Ligands

IHH ×4

Waters ×220

* Residue conservation analysis

PDB id:

3f6x

Name:

Transferase

Title:

C-src kinase domain in complex with small molecule inhibitor

Structure:

Proto-oncogene tyrosine-protein kinase src. Chain: a, b, c, d. Fragment: unp residues 251-533. Synonym: pp60c-src, p60-src, c-src. Engineered: yes

Source:

Gallus gallus. Bantam,chickens. Organism_taxid: 9031. Gene: src. Expressed in: escherichia coli. Expression_system_taxid: 562.

Resolution:

2.35Å R-factor: 0.234 R-free: 0.266

Authors:

M.A.Seeliger,A.V.Statsuk,D.J.Maly,P.Z.Patrick,J.Kuriyan,K.M.Shokat

Key ref:

A.V.Statsuk et al. (2008). Tuning a three-component reaction for trapping kinase substrate complexes. J Am Chem Soc, 130, 17568-17574. PubMed id: 19053485

Date:

06-Nov-08 Release date: 09-Dec-08

Protein chains

P00523  (SRC_CHICK) -  Proto-oncogene tyrosine-protein kinase Src from Gallus gallus

Seq: 533 a.a.

Struc: 264 a.a.

Enzyme reactions

• Enzyme class: E.C.2.7.10.2 - non-specific protein-tyrosine kinase.
• Reaction: L-tyrosyl-[protein] + ATP = O-phospho-L-tyrosyl-[protein] + ADP + H⁺

Molecule diagrams generated from .mol files obtained from the KEGG ftp site

Added reference

J Am Chem Soc 130:17568-17574 (2008)

PubMed id: 19053485

Tuning a three-component reaction for trapping kinase substrate complexes.

A.V.Statsuk, D.J.Maly, M.A.Seeliger, M.A.Fabian, W.H.Biggs, D.J.Lockhart, P.P.Zarrinkar, J.Kuriyan, K.M.Shokat.

ABSTRACT

The upstream protein kinases responsible for thousands of phosphorylation events in the phosphoproteome remain to be discovered. We developed a three-component chemical reaction which converts the transient noncovalent substrate-kinase complex into a covalently cross-linked product by utilizing a dialdehyde-based cross-linker, 1. Unfortunately, the reaction of 1 with a lysine in the kinase active site and an engineered cysteine on the substrate to form an isoindole cross-linked product could not be performed in the presence of competing cellular proteins due to nonspecific side reactions. In order to more selectively target the cross-linker to protein kinases in cell lysates, we replaced the weak, kinase-binding adenosine moiety of 1 with a potent protein kinase inhibitor scaffold. In addition, we replaced the o-phthaldialdehyde moiety in 1 with a less-reactive thiophene-2,3-dicarboxaldehyde moiety. The combination of these two structural modifications provides for cross-linking of a cysteine-containing substrate to its corresponding kinase in the presence of competing cellular proteins.