Article (Scientific journals)
Development of a Genetically Encoded and Potent PDE6D Inhibitor.
Gómez-Mulas, Atanasio; SCHAFFNER-RECKINGER, Elisabeth; Peeters, Hanne et al.
2025In Chembiochem: A European Journal of Chemical Biology, p. 202500739
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Keywords :
PDE6D; RAS; RASopathy; cancer; inhibitors; Biochemistry; Molecular Medicine; Molecular Biology; Organic Chemistry
Abstract :
[en] PDE6D is a trafficking chaperone of prenylated proteins, such as small GTPases. Several small molecule inhibitors have been developed against it, given that the oncogene K-Ras is one of the cargo proteins. Inhibitor development suffers from the fact that inhibitors against the hydrophobic pocket of PDE6D are typically poorly water-soluble. Herein, the development of genetically encoded inhibitors that are inspired by high-affinity natural cargo of PDE6D is described. The most potent inhibitor, SNAP-STI, encodes merely a farnesylated tetra-peptide, which efficiently blocks PDE6D binding of farnesylated cargo. Direct comparison with small molecule PDE6D inhibitors suggests its higher potency. It is shown that inhibition of K-Ras membrane anchorage and K-RasG12C-dependent MAPK signaling by SNAP-STI is weak, consistent with what is observed after PDE6D knockdown. The data therefore further support that PDE6D is not a suitable surrogate target for efficient inhibition of K-Ras membrane anchorage and MAPK-activity. Nonetheless, by exploiting contacts at the pocket entry, a generalizable strategy to design high-affinity PDE6D inhibitors is established, providing powerful tools for PDE6D biology and target validation.
Disciplines :
Biochemistry, biophysics & molecular biology
Author, co-author :
Gómez-Mulas, Atanasio ;  Cancer Cell Biology and Drug Discovery Group, Department of Life Sciences and Medicine, University of Luxembourg, 2 place de l'Université, 4365, Esch-sur-Alzette, Luxembourg
SCHAFFNER-RECKINGER, Elisabeth  ;  University of Luxembourg > Faculty of Science, Technology and Medicine (FSTM) > Department of Life Sciences and Medicine (DLSM)
Peeters, Hanne ;  The Mechanistic Molecular Biochemistry Group, Department of Chemistry, KU Leuven, Celestijnenlaan 200G, 3001, Heverlee, Belgium
CHIPPALKATTI, Rohan  ;  University of Luxembourg > Faculty of Science, Technology and Medicine > Department of Life Sciences and Medicine > Team Daniel ABANKWA
DAUTBASIC, Arnela  ;  University of Luxembourg > Faculty of Humanities, Education and Social Sciences (FHSE) > Department of Humanities (DHUM) > Multilingualism
Smith, Matthew James ;  Institute for Research in Immunology and Cancer, Pavillon Marcelle-Coutu, Université de Montréal, 2950 Chemin de Polytechnique, Montréal, Québec, H3T 1J4, Canada ; Programmes de biologie moléculaire, Université de Montréal, Montreal, Québec, H3C 3J7, Canada ; Department of Pathology and Cell Biology, Faculty of Medicine, Université de Montréal, Montréal, Québec, H3T 1J4, Canada
Ismail, Shehab ;  The Mechanistic Molecular Biochemistry Group, Department of Chemistry, KU Leuven, Celestijnenlaan 200G, 3001, Heverlee, Belgium
ABANKWA, Daniel  ;  University of Luxembourg
External co-authors :
yes
Language :
English
Title :
Development of a Genetically Encoded and Potent PDE6D Inhibitor.
Publication date :
18 November 2025
Journal title :
Chembiochem: A European Journal of Chemical Biology
ISSN :
1439-4227
eISSN :
1439-7633
Publisher :
John Wiley and Sons Inc, Germany
Pages :
e202500739
Peer reviewed :
Peer Reviewed verified by ORBi
Funding text :
This work was supported by the Luxembourg National Research Fund (FNR) grants AFR/23/17112420/Bil_ABANKWA_SPREDCanUL2 to D.K.A. and M.J.S., INTER/FWO/23/18086068 molGluRAS2 to D.K.A., and FWO grant G042824N to S.I. M.J.S. holds a Canada Research Chair (CRC) in Cancer Signalling and Structural Biology.
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