Dual Inhibition of MDM2 and BET Cooperate to Eradicate Acute Myeloid Leukemia

Latif, Anne-Louise; Cole, John; Campos, Joana; Clark, W.R.K.; McGarry, Lynn; Brock, Claire; Newcombe, Ashley; Keeshan, Karen; Copland, Mhairi; Adams, Peter

doi:10.1182/blood.v126.23.674.674

Cited by 1 publication

(1 citation statement)

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“…Furthermore, Hh activation modulates NUMB-p53 responses, therefore, Hh suppression will subsequently alter p53 target genes; p53 is referred to as the guardian of the genome, therefore, careful evaluation of modulation of its function needs to be gained [61,62]. p53 as a modulatory target in leukaemia is an area which is becoming of increasing interest; both in CML [63] and AML [64].…”

Section: Hedgehog Signallingmentioning

confidence: 99%

Approaches for targeting self-renewal pathways in cancer stem cells: implications for hematological treatments

Horne

Copland

2017

Expert Opinion on Drug Discovery

Self Cite

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Self-renewal is considered a defining property of stem cells. Self-renewal is essential in embryogenesis and normal tissue repair and homeostasis. However, in cancer, self-renewal pathways, e.g. WNT, NOTCH, Hedgehog and BMP, frequently become de-regulated in stem cells, or more mature progenitor cells acquire self-renewal properties, resulting in abnormal tissue growth and tumorigenesis. Areas covered: This review considers the conserved embryonic self-renewal pathways, including WNT, NOTCH, Hedgehog and BMP. The article describes recent advances in our understanding of these pathways in leukemia and, more specifically, leukemia stem cells (LSC), how these pathways cross-talk and interact with the LSC microenvironment, and discusses the clinical implications and potential therapeutic strategies, both in preclinical and in clinical trials for hematological malignancies. Expert opinion: The conserved embryonic self-renewal pathways are frequently de-regulated in cancer stem cells (CSC), including LSCs. There is significant cross-talk between self-renewal pathways, and their downstream targets, and the microenvironment. Effective targeting of these pathways is challenging due to cross-talk, and importantly, because these pathways are important for normal stem cells as well as CSC, adverse effects on normal tissues may mean a therapeutic window cannot be identified. Nonetheless, several agents targeting these pathways are currently in clinical trials in hematological malignancies.

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