Discovery and Optimization of Pyrazolopyrimidine Sulfamates as ATG7 Inhibitors

Shih-Chung Huang,Sharmila Adhikari,James E. Brownell,Emily F. Calderwood,Jouhara Chouitar,Natalie Roy DAmore,Dylan England,Klaudia Foley,Sean J. Harrison,Patrick J. LeRoy,David Lok,Anna Lublinsky,Li-Ting Ma,Saurabh Menon,Yu Yang,Ji Zhang,Alexandra E. Gould

Discovery and Optimization of Pyrazolopyrimidine Sulfamates as ATG7 Inhibitors

2020

Shih-Chung Huang
Sharmila Adhikari
James E. Brownell
Emily F. Calderwood
Jouhara Chouitar
Natalie Roy DAmore
Dylan England
Klaudia Foley
Sean J. Harrison
Patrick J. LeRoy
David Lok
Anna Lublinsky
Li-Ting Ma
Saurabh Menon
Yu Yang
Ji Zhang
Alexandra E. Gould

Abstract Autophagy is postulated to be required by cancer cells to survive periods of metabolic and/or hypoxic stress. ATG7 is the E1 enzyme that is required for activation of Ubl conjugation pathways involved in autophagosome formation. This article describes the design and optimization of pyrazolopyrimidine sulfamate compounds as potent and selective inhibitors of ATG7. Cellular levels of the autophagy markers, LC3B and NBR1, are regulated following treatment with these compounds.

Keywords:

Chemistry
hypoxic stress
Autophagy
Autophagosome formation
Pyrazolopyrimidine
Cell biology
Enzyme
Cancer cell

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