| Literature DB >> 34127794 |
Yuki Nishida1, Ran Zhao1, Lauren E Heese1, Hiroki Akiyama1, Shreya Patel1, Alex M Jaeger2, Rodrigo O Jacamo1, Kensuke Kojima1,3, Man Chun John Ma4, Vivian R Ruvolo1, Dhruv Chachad1, William Devine5, Susan Lindquist2, R Eric Davis4, John A Porco5, Luke Whitesell2,6, Michael Andreeff7, Jo Ishizawa8.
Abstract
Eukaryotic initiation factor 4A (eIF4A), the enzymatic core of the eIF4F complex essential for translation initiation, plays a key role in the oncogenic reprogramming of protein synthesis, and thus is a putative therapeutic target in cancer. As important component of its anticancer activity, inhibition of translation initiation can alleviate oncogenic activation of HSF1, a stress-inducible transcription factor that enables cancer cell growth and survival. Here, we show that primary acute myeloid leukemia (AML) cells exhibit the highest transcript levels of eIF4A1 compared to other cancer types. eIF4A inhibition by the potent and specific compound rohinitib (RHT) inactivated HSF1 in these cells, and exerted pronounced in vitro and in vivo anti-leukemia effects against progenitor and leukemia-initiating cells, especially those with FLT3-internal tandem duplication (ITD). In addition to its own anti-leukemic activity, genetic knockdown of HSF1 also sensitized FLT3-mutant AML cells to clinical FLT3 inhibitors, and this synergy was conserved in FLT3 double-mutant cells carrying both ITD and tyrosine kinase domain mutations. Consistently, the combination of RHT and FLT3 inhibitors was highly synergistic in primary FLT3-mutated AML cells. Our results provide a novel therapeutic rationale for co-targeting eIF4A and FLT3 to address the clinical challenge of treating FLT3-mutant AML.Entities:
Mesh:
Substances:
Year: 2021 PMID: 34127794 PMCID: PMC8764661 DOI: 10.1038/s41375-021-01308-z
Source DB: PubMed Journal: Leukemia ISSN: 0887-6924 Impact factor: 12.883