Tracing the origins of relapse in acute myeloid leukaemia to stem cells

Shlush, Liran I.; Mitchell, Amanda; Heisler, Lawrence E.; Abelson, Sagi; Ng, Stanley; Trotman-Grant, Aaron C.; Medeiros, Jessie J. F.; Rao-Bhatia, Abilasha; Jaciw-Zurakowsky, Ivana; Marke, René; McLeod, Jessica; Doedens, Monica; Bader, Gary D.; Voisin, Véronique; Xu, Changjiang; Mcpherson, John Douglas; Hudson, Thomas J.; Wang, Jean; Minden, Mark D.; Dick, John E.

doi:10.1038/nature22993

Cited by 462 publications

(461 citation statements)

References 30 publications

Supporting

Mentioning

443

Contrasting

Unclassified

Order By: Relevance

“…One important conclusion of several of these studies is that CSCs display molecular and functional heterogeneity. Interestingly, this heterogeneity seems to be established early during tumorigenesis because genetically distinct CSC sub-clones are already present in primary tumours, some of which fade or become dominant during tumour progression and response to chemotherapy (Ben-David et al, 2017; Shlush et al, 2017; Zehir et al, 2017). However, it is still a matter of debate whether all cells capable of initiating and promoting primary tumour growth are equally competent to initiate metastasis.…”

Section: Metabolic Heterogeneity Of Cancer Stem Cellsmentioning

confidence: 99%

“…In addition, epidermal stem cells that lack Dnmt3A and 3B upregulate a unique lipid transcriptional network that is associated with CD36 + MICs, and are consequently much more predisposed to generating metastatic epidermal tumours (Pascual et al, 2017; Rinaldi et al, 2017). Considering that the genes encoding Dnmt3a and TET proteins are among the most frequently mutated in human cancers (Shlush et al, 2017; Zehir et al, 2017), it will be interesting to study how their mutations influence tumour metabolism, and vice versa , during metastatic progression.…”

Section: Metabolism-driven Epigenetic Alterations In Cancermentioning

confidence: 99%

See 1 more Smart Citation

The contributions of cancer cell metabolism to metastasis

Pascual

Domínguez

Benitah

2018

Disease Models &Amp; Mechanisms

View full text Add to dashboard Cite

Metastasis remains the leading cause of cancer-related deaths worldwide, and our inability to identify the tumour cells that colonize distant sites hampers the development of effective anti-metastatic therapies. However, with recent research advances we are beginning to distinguish metastasis-initiating cells from their non-metastatic counterparts. Importantly, advances in genome sequencing indicate that the acquisition of metastatic competency does not involve the progressive accumulation of driver mutations; moreover, in the early stages of tumorigenesis, cancer cells harbour combinations of driver mutations that endow them with metastatic competency. Novel findings highlight that cells can disseminate to distant sites early during primary tumour growth, remaining dormant and untreatable for long periods before metastasizing. Thus, metastatic cells must require local and systemic influences to generate metastases. This hypothesis suggests that factors derived from our lifestyle, such as our diet, exert a strong influence on tumour progression, and that such factors could be modulated if understood. Here, we summarize the recent findings on how specific metabolic cues modulate the behaviour of metastatic cells and how they influence the genome and epigenome of metastatic cells. We also discuss how crosstalk between metabolism and the epigenome can be harnessed to develop new anti-metastatic therapies.

show abstract

Section: Metabolic Heterogeneity Of Cancer Stem Cellsmentioning

confidence: 99%

Section: Metabolism-driven Epigenetic Alterations In Cancermentioning

confidence: 99%

The contributions of cancer cell metabolism to metastasis

Pascual

Domínguez

Benitah

2018

Disease Models &Amp; Mechanisms

View full text Add to dashboard Cite

show abstract

“…Resistance-driving mutations have been linked to enhanced leukemia growth and proliferation, clonal expansion at early stages of tumor development and increased leukemia stem cell activity 20–22 . However, studies of resistance to bacterial antibiotics have uncovered frequent examples of evolutionary trade-offs in which the acquisition of drug resistance is coupled with a reduced fitness phenotype 23 .…”

mentioning

confidence: 99%

Clonal evolution mechanisms in NT5C2 mutant-relapsed acute lymphoblastic leukaemia

Tzoneva

Dieck

Oshima

et al. 2018

Nature

104

View full text Add to dashboard Cite

Relapsed acute lymphoblastic leukemia (ALL) is associated with chemotherapy resistance and poor prognosis1. Gain-of-function mutations in the 5′-nucleotidase, cytosolic II (NT5C2) gene induce resistance to 6-mercaptopurine (6-MP) and are selectively present in relapsed ALL2,3. Yet, the mechanisms involved in NT5C2 mutation-driven clonal evolution during leukemia initiation, disease progression and relapse remain unknown. Using a conditional inducible leukemia model, we demonstrate that expression of Nt5c2 p.R367Q, a highly prevalent relapsed-ALL NT5C2 mutation, induces resistance to chemotherapy with 6-MP at the cost of impaired leukemia cell growth and leukemia-initiating cell activity. The loss of fitness phenotype of Nt5c2+/R367Q mutant cells is associated with excess export of purines to the extracellular space and depletion of the intracellular purine nucleotide pool. Consequently, blocking guanosine synthesis via inosine-5′-monophosphate dehydrogenase (IMPDH) inhibition induced increased cytotoxicity against NT5C2-mutant leukemia lymphoblasts. These results identify NT5C2 mutation-associated fitness cost and resistance to chemotherapy as key evolutionary drivers shaping clonal evolution in relapsed ALL and support a role for IMPDH inhibition in the treatment of ALL.

show abstract

“…Leukemia stem cells (LSCs, also known as leukemia-initiating cells) are believed to not only drive disease initiation, progression, and drug resistance, but also contribute to relapse [101–105]. Elimination of every single LSC is, therefore, essential to a long-term cure.…”

Section: Key Open Questions: Application To Hematologic Disordersmentioning

confidence: 99%

Metabolism as master of hematopoietic stem cell fate

2018

View full text Add to dashboard Cite

HSCs have a fate choice when they divide; they can self-renew, producing new HSCs, or produce daughter cells that will mature to become committed cells. Technical challenges, however, have long obscured the mechanics of these choices. Advances in flow-sorting have made possible the purification of HSC populations, but available HSC-enriched fractions still include substantial heterogeneity, and single HSCs have proven extremely difficult to track and observe. Advances in single-cell approaches, however, have led to the identification of a highly purified population of hematopoietic stem cells (HSCs) that make a critical contribution to hematopoietic homeostasis through a preference for self-renewing division. Metabolic cues are key regulators of this cell fate choice, and the importance of controlling the population and quality of mitochondria has recently been highlighted to maintain the equilibrium of HSC populations. Leukemic cells also demand tightly regulated metabolism, and shifting the division balance of leukemic cells toward commitment has been considered as a promising therapeutic strategy. A deeper understanding of precisely how specific modes of metabolism control HSC fate is, therefore, of great biological interest, and more importantly will be critical to the development of new therapeutic strategies that target HSC division balance for the treatment of hematological disease.

show abstract

Tracing the origins of relapse in acute myeloid leukaemia to stem cells

Cited by 462 publications

References 30 publications

The contributions of cancer cell metabolism to metastasis

The contributions of cancer cell metabolism to metastasis

Clonal evolution mechanisms in NT5C2 mutant-relapsed acute lymphoblastic leukaemia

Metabolism as master of hematopoietic stem cell fate

Contact Info

Product

Resources

About