Bisubstrate-Type Chemical Probes Identify GRP94 as a Potential Target of Cytosine-Containing Adenosine Analogs.

Dany PechalrieuFanny AssematLudovic HalbyMarlene MarcellinPengrong YanKarima ChaouiSahil SharmaGabriela ChiosisOdile Burlet-SchiltzPaola Barbara ArimondoMarie Lopez

Published in: ACS chemical biology (2020)

We synthesized affinity-based chemical probes of cytosine-adenosine bisubstrate analogs and identified several potential targets by proteomic analysis. The validation of the proteomic analysis identified the chemical probe as a specific inhibitor of glucose-regulated protein 94 (GRP94), a potential drug target for several types of cancers. Therefore, as a result of the use of bisubstrate-type chemical probes and a chemical-biology methodology, this work opens the way to the development of a new family of GRP94 inhibitors that could potentially be of therapeutic interest.

Keyphrases

living cells
small molecule
fluorescence imaging
single molecule
molecular docking
emergency department
transcription factor
blood pressure
metabolic syndrome
adipose tissue
skeletal muscle
climate change
young adults
nucleic acid
drug induced
protein kinase
weight loss