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PDBsum entry 5k5x
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PDB id:
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Transferase
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Title:
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Crystal structure of human pdgfra
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Structure:
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Platelet-derived growth factor receptor alpha. Chain: a. Fragment: unp residues 550-696,769-973. Synonym: pdgfr-alpha,alpha platelet-derived growth factor receptor, alpha-type platelet-derived growth factor receptor,cd140 antigen-like family member a,cd140a antigen,platelet-derived growth factor alpha receptor,platelet-derived growth factor receptor 2. Engineered: yes
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Source:
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Homo sapiens. Human. Organism_taxid: 9606. Gene: pdgfra, pdgfr2, rhepdgfra. Expressed in: spodoptera frugiperda. Expression_system_taxid: 7108.
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Resolution:
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2.17Å
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R-factor:
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0.193
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R-free:
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0.224
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Authors:
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X.E.Yan,L.Liang,C.H.Yun
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Key ref:
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L.Liang
et al.
(2016).
Structural and biochemical studies of the PDGFRA kinase domain.
Biochem Biophys Res Commun,
477,
667-672.
PubMed id:
DOI:
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Date:
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24-May-16
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Release date:
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17-Aug-16
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PROCHECK
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Headers
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References
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P16234
(PGFRA_HUMAN) -
Platelet-derived growth factor receptor alpha from Homo sapiens
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Seq:
Struc:
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1089 a.a.
345 a.a.
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Key: |
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PfamA domain |
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Secondary structure |
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CATH domain |
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Enzyme class:
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E.C.2.7.10.1
- receptor protein-tyrosine kinase.
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Reaction:
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L-tyrosyl-[protein] + ATP = O-phospho-L-tyrosyl-[protein] + ADP + H+
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L-tyrosyl-[protein]
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+
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ATP
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=
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O-phospho-L-tyrosyl-[protein]
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+
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ADP
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+
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H(+)
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Molecule diagrams generated from .mol files obtained from the
KEGG ftp site
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DOI no:
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Biochem Biophys Res Commun
477:667-672
(2016)
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PubMed id:
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Structural and biochemical studies of the PDGFRA kinase domain.
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L.Liang,
X.E.Yan,
Y.Yin,
C.H.Yun.
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ABSTRACT
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Platelet-derived growth factor receptor α (PDGFRA) is a Type III receptor
tyrosine kinase, and this kinase is a target for treatment of gastrointestinal
stromal tumors (GIST) as it is frequently mutated in these cancers. Most of the
mutations that cause constitutive activation of PDGFRA occur in either the
activation loop (A-loop) or in the juxtamembrane (JM) domain, such as the
mutations D842V or V561D respectively. Treatment of PDGFRA-mutated GIST with
imatinib is successful in some cases, but the D842V mutation is
imatinib-resistant. To better understand the mechanism of PDGFRA
drug-resistance, we have determined the crystal structure of the PDGFRA kinase
domain in the auto-inhibited form, and studied the kinetics of the D842V
mutation. Auto-inhibited PDGFRA is stabilized by the JM domain, which inserts
into the active site of the kinase. The conserved residue Asp842 makes extensive
contacts with several A-loop residues to maintain PDGFRA in the "DFG
out" conformation, which stabilizes the kinase in the inactive state and
facilitates the binding of imatinib. The D842V mutation would therefore be
expected to activate the kinase and hinder the binding of drug through
destabilizing the "DFG out" conformation. Furthermore, our kinetic
data show that drug resistance in the D842V mutation may also in part result
from its increased affinity for ATP. The PDGFRA kinase domain structure we
report in this study has potential to facilitate development of new agents which
can inhibit this kinase, including both its activating and drug-resistant
mutations.
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