Antileukemic Efficacy of BET Inhibitor in a Preclinical Mouse Model of MLL-AF4+ Infant ALL

Bardini, Michela; Trentin, Luca; Rizzo, Francesca; Vieri, Margherita; Savino, Angela Maria; Castro, Patricia Garrido; Fazio, Grazia; Roon, Eddy H.J. Van; Kerstjens, Mark; Smithers, Nicholas; Prinjha, Rab K.; Kronnie, Geertruy te; Basso, Giuseppe; Stam, Ronald W.; Pieters, Rob; Biondi, Andrea; Cazzaniga, Giovanni

doi:10.1158/1535-7163.mct-17-1123

Cited by 18 publications

(14 citation statements)

References 55 publications

(70 reference statements)

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“…Earlier studies demonstrated also synergies of BRD inhibitors with other drugs, such as CBP/p300 inhibitors acting synergistically with BET inhibitors as well as cytotoxic agents and dexamethasone in leukemia 34 . In addition, BET inhibitors showed synergy in cancer models in combination with HDAC inhibitors 82–84 as well as kinase and PARP inhibitors 85–87 . The combination of different inhibitors might also be important in overcoming drug resistance which has been observed in cells treated with BET inhibitors 13 .…”

Section: Discussionmentioning

confidence: 99%

A Chemical Toolbox for the Study of Bromodomains and Epigenetic Signaling

Heidenreich

Zhou

et al. 2018

Preprint

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SummaryBromodomains (BRDs) are evolutionary conserved epigenetic protein interaction modules which recognize ("read") acetyl-lysine, however their role(s) in regulating cellular states and their potential as targets for the development of targeted treatment strategies is poorly understood. Here we present a set of 25 chemical probes, selective tool small molecule inhibitors, covering 29 human bromodomain targets. We comprehensively evaluate the selectivity of this probe-set using BROMOscan® and demonstrate the utility of the set using studies of muscle cell differentiation and triple negative breast cancer (TNBC). We identified cross talk between histone acetylation and the glycolytic pathway resulting in a vulnerability of TNBC cell lines to inhibition of BRPF2/3 BRDs under conditions of glucose deprivation or GLUT1 inhibition. This chemical probe set will serve as a resource for future applications in the discovery of new physiological roles of bromodomain proteins in normal and disease states, and as a toolset for bromodomain target validation.

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Section: Discussionmentioning

confidence: 99%

A Chemical Toolbox for the Study of Bromodomains and Epigenetic Signaling

Heidenreich

Zhou

et al. 2018

Preprint

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“…Recruitment of oxidative metabolism seems to also play a role in relapse in B-ALL (Dobson et al, 2020). We impaired MYC activity through inhibition of BET bromodomain proteins -an intervention that slows progression of MLL-driven leukemia -finding that this inhibitor blocked the conversion of CD34to CD34 + cells (Bardini et al, 2018;Dawson et al, 2011;Delmore et al, 2011). Together, our findings reinforce the notion that LICs are plastic and adaptable, providing possible explanations as to why therapies targeting LICs have yet to prove widespread efficacy despite being the object of intense investigation for over two decades (Pollyea and Jordan, 2017;Saygin et al, 2019).…”

Section: Discussionmentioning

confidence: 95%

Single-cell analysis uncovers mechanisms of plasticity in leukemia initiating cells

Morris

Marion

Hughes

et al. 2020

Preprint

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Leukemia initiating cells (LICs) fuel leukemic growth and spark relapse. Previously thought to be primitive and rare, the LIC state may actually be heterogeneous and dynamic, enabling evasion of therapies. Here, we use single-cell transcriptomics to dissect the ontogeny of MLL-rearranged B-lymphoblastic leukemia (MLL-r B-ALL).Although we identify rare transcriptionally and phenotypically primitive LICs, we also observe LICs emerging from more differentiated populations with the capability to replenish the full cellular diversity of MLL-r B-ALL. We find that activation of MYC-driven oxidative phosphorylation controls this process of LIC state conversion.

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“…RUNX1 is known to be a putative target gene of MLL fusions, and was highly expressed in MLL-AF4 ALL cases, when compared with normal bone marrow cells (Guenther et al, 2008; Krivtsov et al, 2008). The BET inhibitor I-BET151, arrested the growth of MLL-AF4 infant leukemic cells in vitro through gene deregulation, including RUNX1 (Bardini et al, 2018).…”

Section: Discussionmentioning

confidence: 99%

Identification of hub genes and molecular mechanisms in infant acute lymphoblastic leukemia withMLLgene rearrangement

Zhang

Cheng

et al. 2019

PeerJ

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Infant acute lymphoblastic leukemia (ALL) with the mixed lineage leukemia (MLL) gene rearrangement (MLL-R) is considered a distinct leukemia from childhood or non-MLL-R infant ALL. To detect key genes and elucidate the molecular mechanisms ofMLL-R infant ALL, microarray expression data were downloaded from the Gene Expression Omnibus (GEO) database, and differentially expressed genes (DEGs) betweenMLL-R and non-MLL-R infant ALL were identified. Gene ontology (GO) and Kyoto Encyclopedia of Genes and Genomes (KEGG) pathway enrichment analyses were carried out. Then, we constructed a protein-protein interaction (PPI) network and identified the hub genes. Finally, drug-gene interactions were mined. A total of 139 cases ofMLL-R infant ALL including 77 (55.4%) fusions withAF4, 38 (27.3%) withENL, 14 (10.1%) withAF9, and 10 (7.2%) other gene fusions were characterized. A total of 236 up-regulated and 84 down-regulated DEGs were identified. The up-regulated DEGs were mainly involved in homophilic cell adhesion, negative regulation of apoptotic process and cellular response to drug GO terms, while down-regulated DEGs were mainly enriched in extracellular matrix organization, protein kinase C signaling and neuron projection extension GO terms. The up-regulated DEGs were enriched in seven KEGG pathways, mainly involving transcriptional regulation and signaling pathways, and down-regulated DEGs were involved in three main KEGG pathways including Alzheimer’s disease, TGF-beta signaling pathway, and hematopoietic cell lineage. The PPI network included 297 nodes and 410 edges, withMYC,ALB,CD44,PTPRCandTNFidentified as hub genes. Twenty-three drug-gene interactions including four up-regulated hub genes and 24 drugs were constructed by Drug Gene Interaction database (DGIdb). In conclusion,MYC,ALB,CD44,PTPRCandTNFmay be potential bio-markers for the diagnosis and therapy ofMLL-R infant ALL.

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Antileukemic Efficacy of BET Inhibitor in a Preclinical Mouse Model of MLL-AF4+ Infant ALL

Cited by 18 publications

References 55 publications

A Chemical Toolbox for the Study of Bromodomains and Epigenetic Signaling

A Chemical Toolbox for the Study of Bromodomains and Epigenetic Signaling

Single-cell analysis uncovers mechanisms of plasticity in leukemia initiating cells

Identification of hub genes and molecular mechanisms in infant acute lymphoblastic leukemia withMLLgene rearrangement

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