| Literature DB >> 33396582 |
Annamaria Sandomenico1, Lorenzo Di Rienzo2, Luisa Calvanese3, Emanuela Iaccarino1, Gabriella D'Auria1,4, Lucia Falcigno1,4, Angela Chambery5, Rosita Russo5, Guido Franzoso6, Laura Tornatore6, Marco D'Abramo7, Menotti Ruvo1, Edoardo Milanetti2,8, Domenico Raimondo9.
Abstract
GADD45β/MKK7 complex is a non-redundant, cancer cell-restricted survival module downstream of the NF-kB survival pathway, and it has a pathogenically critical role in multiple myeloma, an incurable malignancy of plasma cells. The first-in-class GADD45β/MKK7 inhibitor DTP3 effectively kills MM cells expressing its molecular target, both in vitro and in vivo, by inducing MKK7/JNK-dependent apoptosis with no apparent toxicity to normal cells. DTP3 combines favorable drug-like properties, with on-target-specific pharmacology, resulting in a safe and cancer-selective therapeutic effect; however, its mode of action is only partially understood. In this work, we have investigated the molecular determinants underlying the MKK7 interaction with DTP3 by combining computational, NMR, and spectroscopic methods. Data gathered by fluorescence quenching and computational approaches consistently indicate that the N-terminal region of MKK7 is the optimal binding site explored by DTP3. These findings further the understanding of the selective mode of action of GADD45β/MKK7 inhibitors and inform potential mechanisms of drug resistance. Notably, upon validation of the safety and efficacy of DTP3 in human trials, our results could also facilitate the development of novel DTP3-like therapeutics with improved bioavailability or the capacity to bypass drug resistance.Entities:
Keywords: GADD45β; MKK7; STD-NMR; multiple myeloma; protein-ligand interaction
Year: 2020 PMID: 33396582 PMCID: PMC7824710 DOI: 10.3390/biomedicines9010020
Source DB: PubMed Journal: Biomedicines ISSN: 2227-9059