Discovery of Novel Drug-like PHGDH Inhibitors to Disrupt Serine Biosynthesis for Cancer Therapy.
Dingding GaoShuai TangYixin CenLiang YuanXiaojing LanQing-Hua LiGuo-Qiang LinMin HuangPing TianPublished in: Journal of medicinal chemistry (2023)
Being the rate-limiting enzyme within the serine biosynthesis pathway, phosphoglycerate dehydrogenase (PHGDH) is abnormally overexpressed in numerous malignant tumor cells and is a promising target for cancer treatment. Here, we report a series of novel PHGDH inhibitors using a focused compound screening and structural optimization approach. The lead compound D8 displayed good enzymatic inhibitory activity (IC 50 = 2.8 ± 0.1 μM), high binding affinity ( K d = 2.33 μM), and sensitivity to the cell lines with the PHGDH gene amplification or overexpression. Furthermore, D8 was proven to restrict the de novo serine synthesis from glucose within MDA-MB-468 cells. X-ray crystallographic analysis, molecular dynamics simulations, and mutagenesis experiments on PHGDH revealed the binding site at D175 inside the NAD + -binding pocket. Finally, D8 exhibited excellent in vivo pharmacokinetic properties ( F = 82.0%) and exerted evident antitumor efficacy in the PC9 xenograft mouse model.
Keyphrases
- molecular dynamics simulations
- cancer therapy
- mouse model
- protein kinase
- cell cycle arrest
- induced apoptosis
- small molecule
- crispr cas
- drug delivery
- molecular docking
- cell proliferation
- dna binding
- genome wide
- transcription factor
- single cell
- hydrogen peroxide
- copy number
- magnetic resonance
- adipose tissue
- emergency department
- blood glucose
- insulin resistance
- nitric oxide
- dual energy
- drug induced