Subtypes of familial breast tumours revealed by expression and copy number profiling

Waddell, Nicola; Arnold, Jeremy M.; Cocciardi, Sibylle; Silva, Leonard Da; Marsh, Anna; Riley, Joan; Johnstone, Cameron N.; Orloff, Mohammed S.; Assié, Guillaume; Eng, Charis; Reid, Lynne; Keith, Patricia; Yan, Max; Fox, Stephen B.; Devilee, Peter; Godwin, Andrew K.; Hogervorst, Frans B.L.; Couch, Fergus J.; Investigators, kConFab; Grimmond, Sean M.; Flanagan, James M.; Kk, Khanna; Simpson, Peter T.; Lakhani, Sunil R.; Chenevix-Trench, Georgia

doi:10.1007/s10549-009-0653-1

Cited by 92 publications

(128 citation statements)

References 89 publications

(136 reference statements)

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“…Several large and integrative research studies based on expression and copy number profiling of familial BC demonstrated molecular heterogeneity of these tumors similar to sporadic tumors, as well these studies defined molecular subtypes based on markers other than BRCA1 and BRCA2 germline status [11,43,44]. Microarray or immunohistochemical analyses demonstrated that approximately three quarters of BRCA1-related BC are BLBC whereas BRCA2 tumors generally cluster within the luminal A or B groups [43,44,45,46] and non-BRCA1/2 with luminal A tumors [11,44].…”

Section: Blbc and Brca1mentioning

confidence: 98%

“…Microarray or immunohistochemical analyses demonstrated that approximately three quarters of BRCA1-related BC are BLBC whereas BRCA2 tumors generally cluster within the luminal A or B groups [43,44,45,46] and non-BRCA1/2 with luminal A tumors [11,44].…”

Section: Blbc and Brca1mentioning

confidence: 99%

“…BRCA1-related BLBC are TN and frequently positive for Ki67, basal CKs (CK5/6, CK14), TP53, EGFR, P-cadherin [44,47] and with frequent X-chromosome abnormalities [6]. Interesting, the clinical outcomes for women with BLBC and BRCA1-related BC are broadly similar in particular for early (within 5 years) relapse and pattern of metastatic spread.…”

Section: Blbc and Brca1mentioning

confidence: 99%

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Molecular insights on basal-like breast cancer

Dominguez‐Valentin

Silva

Privat

et al. 2012

Breast Cancer Res Treat

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Molecular classification of breast cancer (BC) identified diverse subgroups that encompass distinct biological behaviour and clinical implications, in particular in relation to prognosis, spread, and incidence of recurrence. Basal like breast cancers (BLBC) compose up to 15% of BC and are characterized by lack of estrogen receptor (ER), progesterone receptor (PR), and HER-2 amplification with expression of basal cytokeratins 5/6, 14, 17, epidermal growth factor receptor (EGFR), and/or c-KIT. There is an overlap in definition between triple-negative BC and BLBC due to the triple-negative profile of BLBC. Also, most BRCA1-associated BCs are BLBC, triple negative, and express basal cytokeratins (5/6, 14, 17) and EGFR.There is a link between sporadic BLBC (occurring in women without germline BRCA1 mutations) with dysfunction of the BRCA1 pathway. Despite the molecular and clinical similarities, these subtypes respond differently to neoadjuvant therapy. BLBCs are associated with an aggressive phenotype, high histological grade, poor clinical behavior, and high rates of recurrences and/or metastasis. Their molecular features render these tumors especially refractory to anti-hormonal-based therapies and the overall prognosis of this subset remains poor. In this article the molecular profile, genomic and epigenetic characteristics as well as BRCA1 pathway dysfunction, clinicopathological behavior, and therapeutic options in BLBC are presented, with emphasis on the discordant findings in current literature.

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Section: Blbc and Brca1mentioning

confidence: 98%

Section: Blbc and Brca1mentioning

confidence: 99%

Section: Blbc and Brca1mentioning

confidence: 99%

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Molecular insights on basal-like breast cancer

Dominguez‐Valentin

Silva

Privat

et al. 2012

Breast Cancer Res Treat

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“…Twosided independent Student's t test without equal variance assumption was used to determine p-values (*, P < 0.05; **, P < 0.01). For analysis of gene expression microarray in primary human breast tumors, box plots and dot plots were performed on three publicly available datasets of BRCA1 mutated breast tumors (van 't Veer et al, 2002;Jönsson et al, 2010;Waddell et al, 2010) and on three sporadic breast tumor datasets (Pawitan et al, 2005;Chin et al, 2006;Sabatier et al, 2011), respectively. Tumor subtype classification was determined as described in each study.…”

Section: Statistical Analysesmentioning

confidence: 99%

BRCA1 interacts with Nrf2 to regulate antioxidant signaling and cell survival

Gorrini¹,

Baniasadi²,

Harris³

et al. 2013

J Cell Biol

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Oxidative stress plays an important role in cancer development and treatment. Recent data implicate the tumor suppressor BRCA1 in regulating oxidative stress, but the molecular mechanism and the impact in BRCA1-associated tumorigenesis remain unclear. Here, we show that BRCA1 regulates Nrf2-dependent antioxidant signaling by physically interacting with Nrf2 and promoting its stability and activation. BRCA1-deficient mouse primary mammary epithelial cells show low expression of Nrf2-regulated antioxidant enzymes and accumulate reactive oxygen species (ROS) that impair survival in vivo. Increased Nrf2 activation rescues survival and ROS levels in BRCA1-null cells. Interestingly, 53BP1 inactivation, which has been shown to alleviate several defects associated with BRCA1 loss, rescues survival of BRCA1-null cells without restoring ROS levels. We demonstrate that estrogen treatment partially restores Nrf2 levels in the absence of BRCA1. Our data suggest that Nrf2-regulated antioxidant response plays a crucial role in controlling survival downstream of BRCA1 loss. The ability of estrogen to induce Nrf2 posits an involvement of an estrogen-Nrf2 connection in BRCA1 tumor suppression. Lastly, BRCA1-mutated tumors retain a defective antioxidant response that increases the sensitivity to oxidative stress. In conclusion, the role of BRCA1 in regulating Nrf2 activity suggests important implications for both the etiology and treatment of BRCA1-related cancers.

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“…For example, several observations may be expected to limit the efficiency of the PARP inhibition in BRCA1-and BRCA2-deficient tumors as a synthetic lethal approach. Increase in RAD51 Waddell et al, 2009) and HR can rescue growth defects in BRCA1-deficient cells . Furthermore, the depletion of 53BP1 can rescue BRCA1 deficiency by reactivation of ATM-dependent HR pathway (Bouwman et al, 2010;Bunting et al, 2010).…”

Section: Arrest/senescencementioning

confidence: 99%