| Literature DB >> 35443029 |
Alexander C Lewis1, Victoria S Pope1, Melinda N Tea1, Manjun Li1, Gus O Nwosu1, Thao M Nguyen1,2, Craig T Wallington-Beddoe1,2,3,4, Paul A B Moretti1, Dovile Anderson5, Darren J Creek5, Maurizio Costabile1,6, Saira R Ali1, Chloe A L Thompson-Peach2,7, B Kate Dredge1, Andrew G Bert1, Gregory J Goodall1, Paul G Ekert8,9,10, Anna L Brown1,2,11, Richard D'Andrea1, Nirmal Robinson1, Melissa R Pitman1,12, Daniel Thomas2,7,13, David M Ross1,2,3,4,7,14, Briony L Gliddon1, Jason A Powell1,2, Stuart M Pitson1,2,12.
Abstract
Inducing cell death by the sphingolipid ceramide is a potential anticancer strategy, but the underlying mechanisms remain poorly defined. In this study, triggering an accumulation of ceramide in acute myeloid leukemia (AML) cells by inhibition of sphingosine kinase induced an apoptotic integrated stress response (ISR) through protein kinase R-mediated activation of the master transcription factor ATF4. This effect led to transcription of the BH3-only protein Noxa and degradation of the prosurvival Mcl-1 protein on which AML cells are highly dependent for survival. Targeting this novel ISR pathway, in combination with the Bcl-2 inhibitor venetoclax, synergistically killed primary AML blasts, including those with venetoclax-resistant mutations, as well as immunophenotypic leukemic stem cells, and reduced leukemic engraftment in patient-derived AML xenografts. Collectively, these findings provide mechanistic insight into the anticancer effects of ceramide and preclinical evidence for new approaches to augment Bcl-2 inhibition in the therapy of AML and other cancers with high Mcl-1 dependency.Entities:
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Year: 2022 PMID: 35443029 DOI: 10.1182/blood.2021013277
Source DB: PubMed Journal: Blood ISSN: 0006-4971 Impact factor: 25.476