Triple-Negative Breast Cancer: Distinguishing between Basal and Nonbasal Subtypes

Rakha, Emad A.; Elsheikh, Somaia; Aleskandarany, Mohammed A.; Habashi, Hany O.; Green, Andrew; Powe, Desmond G.; El-Sayed, Maysa E.; Benhasouna, Ahmed; Brunet, Jean‐Sébastien; Akslen, Lars A.; Evans, Andy; Blamey, R.W.; Reis‐Filho, Jorge S.; Foulkes, William D.; Ellis, Ian O.

doi:10.1158/1078-0432.ccr-08-2132

Cited by 426 publications

(403 citation statements)

References 51 publications

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“…This subgroup present a greater genetic complexity compared with other BC subtypes, suggesting a greater degree of genetic instability [28,29]. Bergamaschi [30] found that BLBC show the highest frequency of DNA losses and gains compared with others subtypes and also reported that despite of the highest prevalence of genomic aberrations, BLBC show less genomic 8 amplifications than tumors pertaining to other molecular subgroups [10,28,30].…”

Section: Genomic Profiling Of Blbcmentioning

confidence: 92%

“…But some particular recurrent amplifications described in BLBC are approximately two to three times higher than the other subtypes [10,28] and it includes 7p11.2 involving the region of EGFR, 7q31 affecting caveolin 1, and 12p13 being the amplifications of 8p12 and 17q11.2 associated with poor outcomes [31].…”

Section: Genomic Profiling Of Blbcmentioning

confidence: 99%

“…There are several reported biomarkers associated with BLBC as well as putative candidates suitable for immunohistochemical screening (Table 1) [10,11,23], however, currently, there is no specific international consensus on complement biomarkers that can define BLBC.…”

Section: Molecular Profile Of Blbcmentioning

confidence: 99%

“…They represent from 8% up to 37% of all BC cases, depending on the proportion of grade III cases included in the populations studied [10]. BLBC presents frequent mutations in the TP53 gene, evidence of genomic instability, and inactivation of the Rb pathway [11].…”

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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: Genomic Profiling Of Blbcmentioning

confidence: 92%

Section: Genomic Profiling Of Blbcmentioning

confidence: 99%

Section: Molecular Profile Of Blbcmentioning

confidence: 99%

mentioning

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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“…This study was based on a well-characterised cohort of early stage (I-III) primary operable invasive BC (n=1902) from patients enrolled into the Nottingham Tenovus Primary Breast Carcinoma Series between 1987 and 1998, and managed in accordance to a uniform protocol and has been comprehensively studied with a broad range of markers [9,10]. During the follow-up time within this series, distant recurrence had developed in 578/1902 cases (30 %).…”

Section: Patients and Tumoursmentioning

confidence: 99%

Markers of progression in early-stage invasive breast cancer: a predictive immunohistochemical panel algorithm for distant recurrence risk stratification

Aleskandarany

Soria

Green

et al. 2015

Breast Cancer Res Treat

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Accurate distant metastasis (DM) prediction is critical for risk stratification and effective treatment decisions in breast cancer (BC). Many prognostic markers/models based on tissue marker studies are continually emerging using conventional statistical approaches analysing complex/dimensional data association with DM/poor prognosis. However, few of them have fulfilled satisfactory evidences for clinical application. This study aimed at building DM risk assessment algorithm for BC patients.A well-characterised series of early invasive primary operable BC (n=1902), with immunohistochemical (IHC) expression of a panel of biomarkers (n=31) formed the material of this study. Decision tree algorithm was computed using WEKA software, utilising quantitative biomarkers' expression and the absence/presence of distant metastases.Fifteen biomarkers were significantly associated with DM, with six temporal subgroups characterised based on time-to-development of DM ranging from < 1 year to > 15 years of follow-up. Of these 15 biomarkers, 10 had a significant expression pattern where Ki67LI, HER2, p53, N-cadherin, P-cadherin, PIK3CA and TOMM34 showed significantly higher expressions with earlier development of DM. In contrast, higher expressions of ER, PR, and BCL2, were associated with delayed occurrence of DM. DM prediction algorithm was built utilising cases informative for the 15 significant markers. Four risk groups of patients were characterised. Three markers; p53, HER2 and BCL2 predicted the probability of DM, based on software-generated cut-offs, with a precision rate of 81.1% for positive predictive value and 77.3%, for the negative predictive value.This algorithm reiterates the reported prognostic values of these three markers and underscores their central biologic role in BC progression. Further independent validation of this pruned panel of biomarkers is therefore warranted.3

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