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PDBsum entry 4p4c
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protein ligands links
Transferase/transferase inhibitor PDB id
4p4c

 

 

 

 

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JSmol PyMol  
Contents
Protein chain
266 a.a.
Ligands
25Q
Waters ×274
PDB id:
4p4c
Name: Transferase/transferase inhibitor
Title: Human epha3 kinase domain in complex with quinoxaline derivatives
Structure: Eph receptor a3. Chain: a. Fragment: kinase domain. Engineered: yes
Source: Homo sapiens. Human. Organism_taxid: 9606. Gene: epha3. Expressed in: escherichia coli. Expression_system_taxid: 469008.
Resolution:
1.60Å     R-factor:   0.179     R-free:   0.202
Authors: J.Dong,A.Caflisch
Key ref: A.Unzue et al. (2014). Pyrrolo[3,2-b]quinoxaline derivatives as types I1/2 and II Eph tyrosine kinase inhibitors: structure-based design, synthesis, and in vivo validation. J Med Chem, 57, 6834-6844. PubMed id: 25076195 DOI: 10.1021/jm5009242
Date:
12-Mar-14     Release date:   13-Aug-14    
PROCHECK
Go to PROCHECK summary
 Headers
 References

Protein chain
Pfam   ArchSchema ?
P29320  (EPHA3_HUMAN) -  Ephrin type-A receptor 3 from Homo sapiens
Seq:
Struc: 		 
Seq:
Struc: 		983 a.a.
266 a.a.
Key:    PfamA domain  Secondary structure  CATH domain

 Enzyme reactions 
   Enzyme class: E.C.2.7.10.1  - receptor protein-tyrosine kinase.
[IntEnz]   [ExPASy]   [KEGG]   [BRENDA]
      Reaction: L-tyrosyl-[protein] + ATP = O-phospho-L-tyrosyl-[protein] + ADP + H+
L-tyrosyl-[protein]
 + ATP
 = O-phospho-L-tyrosyl-[protein]
Bound ligand (Het Group name = 25Q)
matches with 40.54% similarity 		+ ADP
 + H(+)
Molecule diagrams generated from .mol files obtained from the KEGG ftp site

 

 
    Added reference    
 
 
DOI no: 10.1021/jm5009242 J Med Chem 57:6834-6844 (2014)
PubMed id: 25076195  
 
 
Pyrrolo[3,2-b]quinoxaline derivatives as types I1/2 and II Eph tyrosine kinase inhibitors: structure-based design, synthesis, and in vivo validation.
A.Unzue, J.Dong, K.Lafleur, H.Zhao, E.Frugier, A.Caflisch, C.Nevado.
 
  ABSTRACT  
 
The X-ray crystal structures of the catalytic domain of the EphA3 tyrosine kinase in complex with two type I inhibitors previously discovered in silico (compounds A and B) were used to design type I1/2 and II inhibitors. Chemical synthesis of about 25 derivatives culminated in the discovery of compounds 11d (type I1/2), 7b, and 7g (both of type II), which have low-nanomolar affinity for Eph kinases in vitro and a good selectivity profile on a panel of 453 human kinases (395 nonmutant). Surface plasmon resonance measurements show a very slow unbinding rate (1/115 min) for inhibitor 7m. Slow dissociation is consistent with a type II binding mode in which the hydrophobic moiety (trifluoromethyl-benzene) of the inhibitor is deeply buried in a cavity originating from the displacement of the Phe side chain of the so-called DFG motif as observed in the crystal structure of compound 7m. The inhibitor 11d displayed good in vivo efficacy in a human breast cancer xenograft.
 

 

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