Proteogenomic analysis of Inhibitor of Differentiation 4 (ID4) in basal-like breast cancer

Baker, Laura A.; Holliday, Holly; Roden, Daniel; Wu, Sunny Z.; Junankar, Simon; Sérandour, Aurélien A.; Mohammed, Hisham; Nair, Radhika; Sankaranarayanan, Geetha; Law, Andrew M. K.; McFarland, Andrea; Simpson, Peter T.; Lakhani, Sunil R.; Dodson, Eoin; Selinger, Christina; Anderson, Lyndal; Samimi, Goli; Hacker, Neville F.; Lim, Elgene; Ormandy, Christopher J.; Naylor, Matthew J.; Simpson, Kaylene J.; Nikolić, Iva; O’Toole, Sandra A.; Kaplan, Warren; Cowley, Mark J.; Carroll, Jason S.; Molloy, Mark P.; Swarbrick, Alexander

doi:10.21203/rs.3.rs-16182/v2

Cited by 2 publications

(2 citation statements)

References 46 publications

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“…MDC1 is also a tumor suppressor in tumorigenesis models, such as in Mdc1-knockout mice which show increased tumorigenesis due to increased genomic instability [51][52][53][54]. MDC1 also functions as a tumor suppressor in DDR in ER-negative breast cancer, where MDC1 links ID4 to the BRCA1 DDR network [55]. However, our data contrast the tumor suppressor roles of MDC1 in DDR, and instead suggest an oncogenic role in mediating ER function and ERmediated proliferation.…”

Section: Mdc1 Protein Is Differentially Expressed In Er+ Ilc Tumorscontrasting

confidence: 59%

Mediator of DNA damage checkpoint 1 (MDC1) is a novel estrogen receptor co-regulator in invasive lobular carcinoma of the breast

Bordeaux

Sottnik

Mehrotra

et al. 2020

Preprint

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Invasive lobular carcinoma (ILC) is the most common histological subtype of breast cancer, and nearly all ILC tumors express estrogen receptor alpha (ER). However, clinical and laboratory data suggest ILC are strongly estrogen-driven but not equally sensitive to anti-estrogen therapies. We hypothesized that ILC-specific ER transcriptional co-regulators mediate ER functions in ILC and anti-estrogen resistance, and profiled ER-associated proteins by mass spectrometry. Three ER+ ILC cell lines, MDA MB 134VI, SUM44PE, and BCK4, were compared to published data from ER+ invasive ductal carcinoma (IDC) cell lines, and we examined whether siRNA knockdown of identified proteins suppressed ER-driven proliferation in ILC cells. This approach found mediator of DNA damage checkpoint 1 (MDC1), a key tumor suppressor in DNA damage response (DDR), as a putative novel ER co-regulator in ILC. We confirmed ER:MDC1 interaction was specific to ILC cell lines versus IDC cells, and found MDC1 knockdown suppressed ILC cell proliferation and suppressed tamoxifen resistance in MDA MB 134VI. Using RNA-sequencing, we found that in ILC cells, MDC1 knockdown broadly dysregulates the estrogen-driven ER transcriptome, with ER:MDC1 target genes enriched for hormone-response-elements in their promoter regions. Importantly, our data are inconsistent with MDC1 regulating ER via MDC1 DDR and tumor suppressor functions, but instead suggest a novel oncogenic role for MDC1 in mediating ER transcriptional activity as a co-regulator. Supporting this, in breast tumor tissue microarrays MDC1 protein was frequently low or absent in IDC or ER-ILC, but MDC1 loss is rare in ER+ ILC. ER:MDC1 interaction and MDC1 co-regulator functions may underlie cell type-specific ER functions in ILC, and serve as important biomarkers and therapeutic targets to overcome anti-estrogen resistance in ILC.

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Section: Mdc1 Protein Is Differentially Expressed In Er+ Ilc Tumorscontrasting

confidence: 59%

Mediator of DNA damage checkpoint 1 (MDC1) is a novel estrogen receptor co-regulator in invasive lobular carcinoma of the breast

Bordeaux

Sottnik

Mehrotra

et al. 2020

Preprint

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“…Cytokines and chemokines in tumor microenvironment and epigenetic and transcription factors are other commonly used tools to convert non-stem cancer cells into iCSCs. Inhibitor of differentiation 4 (ID4) was found to dedifferentiate non-stem glioma cells into glioma stem cells [105] and also associated with a stem-like poor prognosis phenotype in triple negative breast cancer [106] . Several reports indicate that dedifferentiation-redifferentiation process is critical for carcinogenesis, selective survival of tumor stem cells that drives invasion and metastases.…”

Section: Dedifferentiation Drug Resistance and Targeted Purging Of Cmentioning

confidence: 99%

Transitional dynamics of cancer stem cells in invasion and metastasis

Richard

Kumar

Pillai

2021

Translational Oncology

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Highlights The cell-of-origin of early and late disseminating, metastatic clones determines tumor aggressiveness. Cellular senescence and microenvironmental cues also promote collective invasion and acquired stemness as a dynamic state in non-senescent tumor cells. Cancer stem cells instigate heterogeneity by existing in a reversible state of dormancy, quiescence, aneuploidy, stemness and drug resistance.

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Proteogenomic analysis of Inhibitor of Differentiation 4 (ID4) in basal-like breast cancer

Cited by 2 publications

References 46 publications

Mediator of DNA damage checkpoint 1 (MDC1) is a novel estrogen receptor co-regulator in invasive lobular carcinoma of the breast

Mediator of DNA damage checkpoint 1 (MDC1) is a novel estrogen receptor co-regulator in invasive lobular carcinoma of the breast

Transitional dynamics of cancer stem cells in invasion and metastasis

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