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  4. A C-Degron Structure-Based Approach for the Development of Ligands Targeting the E3 Ligase TRIM7
 
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2024
Journal Article
Title

A C-Degron Structure-Based Approach for the Development of Ligands Targeting the E3 Ligase TRIM7

Abstract
TRIM7 is a ubiquitin E3 ligase with key regulatory functions, mediating viral infection, tumor biology, innate immunity, and cellular processes, such as autophagy and ferroptosis. It contains a PRYSPRY domain that specifically recognizes degron sequences containing C-terminal glutamine. Ligands that bind to the TRIM7 PRYSPRY domain may have applications in the treatment of viral infections, as modulators of inflammation, and in the design of a new class of PROTACs (PROteolysis TArgeting Chimeras) that mediate the selective degradation of therapeutically relevant proteins (POIs). Here, we developed an assay toolbox for the comprehensive evaluation of TRIM7 ligands. Using TRIM7 degron sequences together with a structure-based design, we developed the first series of peptidomimetic ligands with low micromolar affinity. The terminal carboxylate moiety was required for ligand activity but prevented cell penetration. A prodrug strategy using an ethyl ester resulted in enhanced permeability, which was evaluated using confocal imaging.
Author(s)
Muñoz Sosa, Christian J.
Lenz, Christopher
Hamann, Anton
Farges, Frederic
Dopfer, Johannes
Krämer, Andreas
Cherkashyna, Veronika
Tarnovskiy, Andrey
Moroz, Yurii S.
Proschak, Eugen
Fraunhofer-Institut für Translationale Medizin und Pharmakologie ITMP  
Němec, Václav
Müller, Susanne
Saxena, Krishna
Knapp, Stefan
Journal
ACS chemical biology  
DOI
10.1021/acschembio.4c00301
Language
English
Fraunhofer-Institut für Translationale Medizin und Pharmakologie ITMP  
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