Structure-Based Design and Synthesis of Potent and Selective KRAS G12D Inhibitors.

Hengmiao ChengPuhui LiPing ChenAdriana IrimiaJae Hyun BaeAlexei BroounPatrick FaganRichard LamBingzhen LinJingchuan ZhangXuejun ZhanXu WuNan XieGary ChiangRobert ShoemakerJean-Michel Vernier

Published in: ACS medicinal chemistry letters (2023)

KRAS G12D mutation has been found in approximately 45% of pancreatic ductal adenocarcinoma (PDAC) cases, making it an attractive therapeutic target. Through structure-based drug design, a series of potent and selective KRAS G12D inhibitors were designed. The lead compound, ERAS-5024, inhibited ERK1/2 phosphorylation and cell proliferation in three-dimensional Cell-Titer Glo assays in AsPC-1 PDAC cells with single-digit nanomolar potency and caused tumor regression in the in vivo efficacy studies. We describe here the details of the design and synthesis program that led to the discovery of ERAS-5024.

Keyphrases

cell proliferation
wild type
induced apoptosis
high throughput
signaling pathway
small molecule
pi k akt
single cell
anti inflammatory
cell cycle arrest
cell therapy
stem cells
cell cycle
quality improvement
oxidative stress
cell death
mesenchymal stem cells
endoplasmic reticulum stress
drug induced