Leukemia stem cells, however, are dependent on a protein complex called polycomb repressive complex 1, or PRC1, which interacts with chromatin and turns genes off.
Now a team of researchers led by Tomasz Cierpicki, Ph.D., and Jolanta Grembecka, Ph.D., from the University of Michigan has developed the first small-molecule inhibitors of PRC1 — a first step toward developing a potential new therapeutic approach to treating acute myeloid leukemia by shutting down the activity of leukemia stem cells.
These inhibitors demonstrate activity in leukemia cells and patient samples, as reported in Nature Chemical Biology, and also open new opportunities to study the development of leukemia at the molecular level.
“Our lead compound, RB-3, represents an attractive and unique agent for studying PRC1 biology,” said Cierpicki, an associate professor of biophysics and pathology at U-M. “This work demonstrates that directly targeting the activity of PRC1 is indeed feasible and could lay the groundwork for the development of new pharmaceutical agents for leukemia and possibly other cancers.”
The study was a close collaboration between his lab and the lab of co-senior author Grembecka, an associate professor of pathology at Michigan Medicine and co-director of the developmental therapeutics program at the U-M Rogel Cancer Center.
Paper cited: “Small molecule inhibitors targeting Polycomb repressive complex 1 RING domain,” Nature Chemical Biology. DOI: 10.1038/s41589-021-00815-5