| Literature DB >> 33769048 |
Markus Hartmann1, Jessica Huber2, Jan S Kramer1, Jan Heering3, Larissa Pietsch4, Holger Stark5,6, Dalibor Odadzic5, Iris Bischoff7, Robert Fürst7, Martin Schröder1, Masato Akutsu8, Apirat Chaikuad1, Volker Dötsch2, Stefan Knapp1,5, Ricardo M Biondi4, Vladimir V Rogov1,2, Ewgenij Proschak1,3,5.
Abstract
Autophagy is the common name for a number of lysosome-based degradation pathways of cytosolic cargos. The key components of autophagy are members of Atg8 family proteins involved in almost all steps of the process, from autophagosome formation to their selective fusion with lysosomes. In this study, we show that the homologous members of the human Atg8 family proteins, LC3A and LC3B, are druggable by a small molecule inhibitor novobiocin. Structure-activity relationship (SAR) studies of the 4-hydroxy coumarin core scaffold were performed, supported by a crystal structure of the LC3A dihydronovobiocin complex. The study reports the first nonpeptide inhibitors for these protein interaction targets and will lay the foundation for the development of more potent chemical probes for the Atg8 protein family which may also find applications for the development of autophagy-mediated degraders (AUTACs).Entities:
Year: 2021 PMID: 33769048 DOI: 10.1021/acs.jmedchem.0c01564
Source DB: PubMed Journal: J Med Chem ISSN: 0022-2623 Impact factor: 7.446