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PDBsum entry 4wbo
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Transferase/transferase inhibitor
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PDB id
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4wbo
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References listed in PDB file
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Key reference
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Title
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Identification and characterization of amlexanox as a g protein-Coupled receptor kinase 5 inhibitor.
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Authors
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K.T.Homan,
E.Wu,
A.Cannavo,
W.J.Koch,
J.J.Tesmer.
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Ref.
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Molecules, 2014,
19,
16937-16949.
[DOI no: ]
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PubMed id
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Abstract
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G protein-coupled receptor kinases (GRKs) have been implicated in human diseases
ranging from heart failure to diabetes. Previous studies have identified several
compounds that selectively inhibit GRK2, such as paroxetine and balanol. Far
fewer selective inhibitors have been reported for GRK5, a target for the
treatment of cardiac hypertrophy, and the mechanism of action of reported
compounds is unknown. To identify novel scaffolds that selectively inhibit GRK5,
a differential scanning fluorometry screen was used to probe a library of 4480
compounds. The best hit was amlexanox, an FDA-approved anti-inflammatory,
anti-allergic immunomodulator. The crystal structure of amlexanox in complex
with GRK1 demonstrates that its tricyclic aromatic ring system forms ATP-like
interactions with the hinge of the kinase domain, which is likely similar to how
this drug binds to IκB kinase ε (IKKε), another kinase known to be inhibited
by this compound. Amlexanox was also able to inhibit myocyte enhancer factor 2
transcriptional activity in neonatal rat ventricular myocytes in a manner
consistent with GRK5 inhibition. The GRK1 amlexanox structure thus serves as a
springboard for the rational design of inhibitors with improved potency and
selectivity for GRK5 and IKKε.
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