TY - JOUR
T1 - Overcoming Paradoxical Kinase Priming by a Novel MNK1 Inhibitor
AU - Bou-Petit, Elisabeth
AU - Hümmer, Stefan
AU - Alarcon, Helena
AU - Slobodnyuk, Konstantin
AU - Cano-Galietero, Marta
AU - Fuentes, Pedro
AU - Guijarro, Pedro J.
AU - Muñoz, María José
AU - Suarez-Cabrera, Leticia
AU - Santamaria, Anna
AU - Estrada-Tejedor, Roger
AU - Borrell, José I.
AU - Ramón Y Cajal, Santiago
N1 - Funding Information:
This work was supported by the Instituto de Salud Carlos III (PI17/02247), (PI20/01687), and CIBERONC (CB16/12/00363). S.R.y.C. acknowledges support from the Generalitat de Catalunya (2017-9015-385045). E. Bou-Petit thanks the Secretaria d’Universitats i Recerca del Departament d’Economia i Coneixement de la Generalitat de Catalunya (2017 FI_B2 00139) and the European Social Funds for her predoctoral fellowship.
Publisher Copyright:
© 2022 American Chemical Society. All rights reserved.
PY - 2022/4/28
Y1 - 2022/4/28
N2 - Targeting the kinases MNK1 and MNK2 has emerged as a valuable strategy in oncology. However, most of the advanced inhibitors are acting in an adenosine triphosphate (ATP)-competitive mode, precluding the evaluation of different binding modes in preclinical settings. Using rational design, we identified and validated the 4,6-diaryl-pyrazolo[3,4-b]pyridin-3-amine scaffold as the core for MNK inhibitors. Signaling pathway analysis confirmed a direct effect of the hit compound EB1 on MNKs, and in line with the reported function of these kinases, EB1 only affects the growth of tumor but not normal cells. Molecular modeling revealed the binding of EB1 to the inactive conformation of MNK1 and the interaction with the specific DFD motif. This novel mode of action appears to be superior to the ATP-competitive inhibitors, which render the protein in a pseudo-active state. Overcoming this paradoxical activation of MNKs by EB1 represents therefore a promising starting point for the development of a novel generation of MNK inhibitors.
AB - Targeting the kinases MNK1 and MNK2 has emerged as a valuable strategy in oncology. However, most of the advanced inhibitors are acting in an adenosine triphosphate (ATP)-competitive mode, precluding the evaluation of different binding modes in preclinical settings. Using rational design, we identified and validated the 4,6-diaryl-pyrazolo[3,4-b]pyridin-3-amine scaffold as the core for MNK inhibitors. Signaling pathway analysis confirmed a direct effect of the hit compound EB1 on MNKs, and in line with the reported function of these kinases, EB1 only affects the growth of tumor but not normal cells. Molecular modeling revealed the binding of EB1 to the inactive conformation of MNK1 and the interaction with the specific DFD motif. This novel mode of action appears to be superior to the ATP-competitive inhibitors, which render the protein in a pseudo-active state. Overcoming this paradoxical activation of MNKs by EB1 represents therefore a promising starting point for the development of a novel generation of MNK inhibitors.
KW - Activated protein-kinases
KW - Initiation-factor 4e
KW - Eif4e phosphorylation
KW - Molecular-dynamics
KW - Translational control
KW - Interacting kinases
KW - Potent
KW - Expression
KW - Discovery
KW - Design
UR - https://www.scopus.com/pages/publications/85128994598
UR - https://www.webofscience.com/api/gateway?GWVersion=2&SrcApp=pure_univeritat_ramon_llull&SrcAuth=WosAPI&KeyUT=WOS:000797573100014&DestLinkType=FullRecord&DestApp=WOS_CPL
UR - http://hdl.handle.net/20.500.14342/4507
U2 - 10.1021/acs.jmedchem.1c01941
DO - 10.1021/acs.jmedchem.1c01941
M3 - Article
C2 - 35417652
AN - SCOPUS:85128994598
SN - 0022-2623
VL - 65
SP - 6070
EP - 6087
JO - Journal of Medicinal Chemistry
JF - Journal of Medicinal Chemistry
IS - 8
ER -