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  •   University of Thessaly Institutional Repository
  • Επιστημονικές Δημοσιεύσεις Μελών ΠΘ (ΕΔΠΘ)
  • Δημοσιεύσεις σε περιοδικά, συνέδρια, κεφάλαια βιβλίων κλπ.
  • View Item
  •   University of Thessaly Institutional Repository
  • Επιστημονικές Δημοσιεύσεις Μελών ΠΘ (ΕΔΠΘ)
  • Δημοσιεύσεις σε περιοδικά, συνέδρια, κεφάλαια βιβλίων κλπ.
  • View Item
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Design and Synthesis of Type-IV Inhibitors of BRAF Kinase That Block Dimerization and Overcome Paradoxical MEK/ERK Activation

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Author
Beneker C.M., Rovoli M., Kontopidis G., Röring M., Galda S., Braun S., Brummer T., McInnes C.
Date
2019
Language
en
DOI
10.1021/acs.jmedchem.8b01288
Keyword
B Raf kinase inhibitor
B Raf kinase
mitogen activated protein kinase
mitogen activated protein kinase kinase kinase
peptide
protein binding
protein kinase inhibitor
Article
binding affinity
controlled study
dimerization
drug design
drug structure
drug synthesis
human
human cell
melanoma cell
proof of concept
signal transduction
cell line
chemistry
dimerization
drug effect
MAPK signaling
metabolism
molecular dynamics
structure activity relation
synthesis
Cell Line
Dimerization
Drug Design
Extracellular Signal-Regulated MAP Kinases
Humans
MAP Kinase Kinase Kinases
MAP Kinase Signaling System
Molecular Dynamics Simulation
Peptides
Protein Binding
Protein Kinase Inhibitors
Proto-Oncogene Proteins B-raf
Structure-Activity Relationship
American Chemical Society
Metadata display
Abstract
Despite the clinical success of BRAF inhibitors like vemurafenib in treating metastatic melanoma, resistance has emerged through "paradoxical MEK/ERK signaling" where transactivation of one protomer occurs as a result of drug inhibition of the other partner in the activated dimer. The importance of the dimerization interface in the signaling potential of wild-type BRAF in cells expressing oncogenic Ras has recently been demonstrated and proposed as a site of therapeutic intervention in targeting cancers resistant to adenosine triphosphate competitive drugs. The proof of concept for a structure-guided approach targeting the dimerization interface is described through the design and synthesis of macrocyclic peptides that bind with high affinity to BRAF and that block paradoxical signaling in malignant melanoma cells occurring through this drug target. The lead compounds identified are type-IV kinase inhibitors and represent an ideal framework for conversion into next-generation BRAF inhibitors through macrocyclic drug discovery. © 2019 American Chemical Society.
URI
http://hdl.handle.net/11615/71559
Collections
  • Δημοσιεύσεις σε περιοδικά, συνέδρια, κεφάλαια βιβλίων κλπ. [19735]

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