Targeting Oncogenic Polyamines in Refractory Pediatric Leukemias Using the Anti-Protozoan Drug Α-Difluoromethylornithine (DFMO) in Combination with GC7 and Aurothioglucose

Hofmann, Bradley; Kannappan, Sunand; Gupta, Meena; Zhang, Chunfen; Chi, Susan; Hanson, Derek; Anderson, Ronald; Narendran, Aru

doi:10.1182/blood-2018-99-117229

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“…The treatment of five AML and five CML patients with DFMO in combination with MGBG led to complete response in one patient and partial response in four ( 100 ). Treating the AML cell line THP1 with DFMO led to PARP, caspase 3, and caspase 7 cleavage indicative of the induction of cell death ( 101 ), Similarly DFMO treatment decreased proliferation of the CML cell line K562 ( 102 ). While the preclinical efficacy of DFMO to reduce intracellular polyamine levels and impair proliferation of myeloid cells ( 103 ) and leukemic cells has effectively been shown, there is no clinical data on its efficacy in myeloid malignancies.…”

Section: Conditionally Essential Amino Acidsmentioning

confidence: 99%

Targeting Amino Acid Metabolic Vulnerabilities in Myeloid Malignancies

et al. 2021

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Tumor cells require a higher supply of nutrients for growth and proliferation than normal cells. It is well established that metabolic reprograming in cancers for increased nutrient supply exposes a host of targetable vulnerabilities. In this article we review the documented changes in expression patterns of amino acid metabolic enzymes and transporters in myeloid malignancies and the growing list of small molecules and therapeutic strategies used to disrupt amino acid metabolic circuits within the cell. Pharmacological inhibition of amino acid metabolism is effective in inducing cell death in leukemic stem cells and primary blasts, as well as in reducing tumor burden in in vivo murine models of human disease. Thus targeting amino acid metabolism provides a host of potential translational opportunities for exploitation to improve the outcomes for patients with myeloid malignancies.

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