| Literature DB >> 34267881 |
Jinyue Ding1, Rajesh Gumpena2, Marc-Olivier Boily1, Alexandre Caron1, Oliver Chong1, Jennifer H Cox1, Valerie Dumais1, Samuel Gaudreault1, Aaron H Graff2, Andrew King1, John Knight3, Renata Oballa1, Jayakumar Surendradoss1, Tim Tang1, Joyce Wu1, W Todd Lowther2, David A Powell1.
Abstract
Both glycolate oxidase (GO) and lactate dehydrogenase A (LDHA) influence the endogenous synthesis of oxalate and are clinically validated targets for treatment of primary hyperoxaluria (PH). We investigated whether dual inhibition of GO and LDHA may provide advantage over single agents in treating PH. Utilizing a structure-based drug design (SBDD) approach, we developed a series of novel, potent, dual GO/LDHA inhibitors. X-ray crystal structures of compound 15 bound to individual GO and LDHA proteins validated our SBDD strategy. Dual inhibitor 7 demonstrated an IC50 of 88 nM for oxalate reduction in an Agxt-knockdown mouse hepatocyte assay. Limited by poor liver exposure, this series of dual inhibitors failed to demonstrate significant PD modulation in an in vivo mouse model. This work highlights the challenges in optimizing in vivo liver exposures for diacid containing compounds and limited benefit seen with dual GO/LDHA inhibitors over single agents alone in an in vitro setting.Entities:
Year: 2021 PMID: 34267881 PMCID: PMC8274068 DOI: 10.1021/acsmedchemlett.1c00196
Source DB: PubMed Journal: ACS Med Chem Lett ISSN: 1948-5875 Impact factor: 4.632