Targeting MYCN-expressing triple-negative breast cancer with BET and MEK inhibitors

Schafer, Johanna M.; Lehmann, Brian D.; Gonzalez-Ericsson, Paula I.; Marshall, Clayton B.; Beeler, J. Scott; Redman, Lindsay N.; Jin, Hailing; Sánchez, Violeta; Stubbs, Matthew C.; Scherle, Peggy; Johnson, Kimberly N.; Sheng, Quanhu; Roland, Joseph T.; Bauer, Joshua A.; Shyr, Yu; Chakravarthy, Bapsi; Mobley, Bret C.; Hiebert, Scott W.; Balko, Justin M.; Sanders, Melinda E.; Liu, Phillip C.C.; Pietenpol, Jennifer A.

doi:10.1126/scitranslmed.aaw8275

Cited by 54 publications

(34 citation statements)

References 79 publications

(91 reference statements)

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“…Altogether, these results support the concept that BET-bromodomain inhibition promotes HR deficiency through depletion of the DNA double stand break resection protein CtIP (C-terminal binding protein (CtBP) interacting protein] [29]. The results also support that simultaneous inhibition of BET and PARP [22], as well as ATR, especially in context of MYC amplified cancers such as this case [30], might result in a robust synthetic lethality in HR-reduced cancer cells.…”

Section: Ex Vivo Dna Repair Targeted Rnai Screeningsupporting

confidence: 78%

Ex vivo analysis of DNA repair targeting in extreme rare cutaneous apocrine sweat gland carcinoma

Mäkelä¹,

Härmä

Fajardo

et al. 2021

Oncotarget

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Cutaneous apocrine carcinoma is an extreme rare malignancy derived from a sweat gland. Histologically sweat gland cancers resemble metastatic mammary apocrine carcinomas, but the genetic landscape remains poorly understood. Here, we report a rare metastatic case with a PALB2 aberration identified previously as a familial susceptibility gene for breast cancer in the Finnish population. As PALB2 exhibits functions in the BRCA1/2-RAD51-dependent homologous DNA recombination repair pathway, we sought to use ex vivo functional screening to explore sensitivity of the tumor cells to therapeutic targeting of DNA repair. Drug screening suggested sensitivity of the PALB2 deficient cells to BET-bromodomain inhibition, and modest sensitivity to DNA-PKi, ATRi, WEE1i and PARPi. A phenotypic RNAi screen of 300 DNA repair genes was undertaken to assess DNA repair targeting in more detail. Core members of the HR and MMEJ pathways were identified to be essential for viability of the cells. RNAi inhibition of RAD52-dependent HR on the other hand potentiated the efficacy of a novel BETi ODM-207. Together these results describe the first ever CAC case with a BRCAness genetic background, evaluate combinatorial DNA repair targeting, and provide a data resource for further analyses of DNA repair targeting in PALB2 deficient cancers.

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Section: Ex Vivo Dna Repair Targeted Rnai Screeningsupporting

confidence: 78%

Ex vivo analysis of DNA repair targeting in extreme rare cutaneous apocrine sweat gland carcinoma

Mäkelä¹,

Härmä

Fajardo

et al. 2021

Oncotarget

View full text Add to dashboard Cite

show abstract

“…Consistently, the part 2 of COLET study was designed to test the combination of cobimetinib, nab-paclitaxel and atezolizumab, with preliminary signs of activity in the PD-L1-positive population 87 . Recently, the concomitant inhibition of MEK and bromodomain and extraterminal motif (BET) has shown synergistic activity in TNBC preclinical models overexpressing the neuroendocrine-associated oncogene MYCN 88 , providing a rationale to explore this combination in patients with MYCN-positive TNBC.…”

Section: Introductionmentioning

confidence: 99%

Practical classification of triple-negative breast cancer: intratumoral heterogeneity, mechanisms of drug resistance, and novel therapies

et al. 2020

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Triple-negative breast cancer (TNBC) is not a unique disease, encompassing multiple entities with marked histopathological, transcriptomic and genomic heterogeneity. Despite several efforts, transcriptomic and genomic classifications have remained merely theoretic and most of the patients are being treated with chemotherapy. Driver alterations in potentially targetable genes, including PIK3CA and AKT, have been identified across TNBC subtypes, prompting the implementation of biomarker-driven therapeutic approaches. However, biomarker-based treatments as well as immune checkpoint inhibitor-based immunotherapy have provided contrasting and limited results so far. Accordingly, a better characterization of the genomic and immune contexture underpinning TNBC, as well as the translation of the lessons learnt in the metastatic disease to the early setting would improve patients’ outcomes. The application of multi-omics technologies, biocomputational algorithms, assays for minimal residual disease monitoring and novel clinical trial designs are strongly warranted to pave the way toward personalized anticancer treatment for patients with TNBC.

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“…About half of all recurrent TNBC express high levels of n-MYC. 119 These n-MYC overexpressing cells appear to be quite sensitive to the combination of the MEK inhibitor trametinib with high dose (500 nM) JQ1. This combination effectively repressed the levels of both n-MYC and MYC as well as ERK/MAPK phosphorylation.…”

Section: Lessons From Clinical Trialsmentioning

confidence: 99%

Achieving clinical success with BET inhibitors as anti-cancer agents

2021

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The transcriptional upregulation of oncogenes is a driving force behind the progression of many tumours. However, until a decade ago, the concept of ‘switching off’ these oncogenic pathways represented a formidable challenge. Research has revealed that members of the bromo- and extra-terminal domain (BET) motif family are key activators of oncogenic networks in a spectrum of cancers; their function depends on their recruitment to chromatin through two bromodomains (BD1 and BD2). The advent of potent inhibitors of BET proteins (BETi), which target either one or both bromodomains, represents an important step towards the goal of suppressing oncogenic networks within tumours. Here, we discuss the biology of BET proteins, advances in BETi design and highlight potential biomarkers predicting their activity. We also outline the logic of incorporating BETi into combination therapies to enhance its efficacy. We suggest that understanding mechanisms of activity, defining predictive biomarkers and identifying potent synergies represents a roadmap for clinical success using BETi.

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Targeting MYCN-expressing triple-negative breast cancer with BET and MEK inhibitors

Cited by 54 publications

References 79 publications

Ex vivo analysis of DNA repair targeting in extreme rare cutaneous apocrine sweat gland carcinoma

Ex vivo analysis of DNA repair targeting in extreme rare cutaneous apocrine sweat gland carcinoma

Practical classification of triple-negative breast cancer: intratumoral heterogeneity, mechanisms of drug resistance, and novel therapies

Achieving clinical success with BET inhibitors as anti-cancer agents

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