Personalizing the treatment of women with early breast cancer: highlights of the St Gallen International Expert Consensus on the Primary Therapy of Early Breast Cancer 2013

Winer, Eric P.; Thürlimann, Beat; Senn, Hans-Jörg; Albain, Kathy S.; André, Fabrice; Bergh, Jonas; Bonnefoi, Hervé; Bretel-Morales, Denisse; Burstein, Harold J.; Cardoso, Fátima; Castiglione‐Gertsch, Monica; Coates, Alan S.; Colleoni, Marco; Costa, Alberto; Curigliano, Giuseppe; Davidson, Nancy E.; Leo, Angelo Di; Ejlertsen, Bent; Forbes, John F.; Gelber, Richard D.; Gnant, Michael; Goldhirsch, Aron; Goodwin, Pamela J.; Goss, Paul E.; Harris, Jay R.; Hayes, Daniel F.; Hudis, Clifford A.; Ingle, James N.; Jassem, Jacek; Jiang, Zefei; Karlsson, Per; Loibl, Sibylle; Morrow, Monica; Namer, M.; Osborne, C. Kent; Partridge, Ann H.; Penault‐Llorca, Frédérique; Perou, Charles M.; Piccart‐Gebhart, Martine; Pritchard, Kathleen I.; Rutgers, Emiel J. T.; Sedlmayer, Felix; Семиглазов, Владимир; Shao, Zhi‐Ming; Smith, Ian; Toi, Masakazu; Varga, Andrea; Untch, Michael; Viale, Giuseppe; Watanabe, Tôru; Wilcken, Nicholas; Wood, William C.

doi:10.1093/annonc/mdt303

Cited by 3,040 publications

(2,882 citation statements)

References 97 publications

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“…Classification of molecular subtypes was based on St Gallen recommendations14 with IHC analysis of ER, PR and Ki‐67, and silver ISH analysis of HER2. The molecular subtypes were defined as follows: luminal A‐like (ER‐positive and PR more than 20 per cent, low Ki‐67 and HER2‐negative), luminal B‐like HER2‐negative (ER‐positive, PR 20 per cent or less and/or high Ki‐67 and HER2‐negative), luminal B‐like HER2‐positive (ER‐positive and/or PR‐positive, any Ki‐67 and HER2‐positive), HER2‐positive (non‐luminal) (ER‐negative, PR‐negative, any Ki‐67 and HER2‐positive) and triple‐negative (ER‐negative, PR‐negative, HER2‐negative, any Ki‐67).…”

Section: Methodsmentioning

confidence: 99%

“…High expression levels of the proliferation marker Ki‐67 are related to poor prognosis12. According to the St Gallen 2011 and 2013 guidelines13, 14, a proxy for the molecular subtype classification based on immunohistochemical analysis and in situ hybridization (ISH) of ER, PR, Ki‐67 and HER2 can be used to divide tumours into four to five main subtypes: luminal A‐like, luminal B‐like (HER2‐positive or HER2‐negative), HER2‐positive (non‐luminal) and triple‐negative breast cancer. This classification is important as it provides prognostic information that guides systemic therapy.…”

Section: Introductionmentioning

confidence: 99%

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St Gallen molecular subtypes in screening-detected and symptomatic breast cancer in a prospective cohort with long-term follow-up

Falck

Röme

Fernö

et al. 2016

British Journal of Surgery

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BackgroundDiagnosis by screening mammography is considered an independent positive prognostic factor, although the data are not fully in agreement. The aim of the study was to explore whether the mode of detection (screening‐detected versus symptomatic) adds prognostic information to the St Gallen molecular subtypes of primary breast cancer, in terms of 10‐year cumulative breast cancer mortality (BCM).MethodsA prospective cohort of patients with primary breast cancer, who had regularly been invited to screening mammography, were included. Tissue microarrays were constructed from primary tumours and lymph node metastases, and evaluated by two independent pathologists. Primary tumours and lymph node metastases were classified into St Gallen molecular subtypes. Cause of death was retrieved from the Central Statistics Office.ResultsA total of 434 patients with primary breast cancer were included in the study. Some 370 primary tumours and 111 lymph node metastases were classified into St Gallen molecular subtypes. The luminal A‐like subtype was more common among the screening‐detected primary tumours (P = 0·035) and corresponding lymph node metastases (P = 0·114) than among symptomatic cancers. Patients with screening‐detected tumours had a lower BCM (P = 0·017), and for those diagnosed with luminal A‐like tumours the 10‐year cumulative BCM was 3 per cent. For patients with luminal A‐like lymph node metastases, there was no BCM. In a stepwise multivariable analysis, the prognostic information yielded by screening detection was hampered by stage and tumour biology.ConclusionThe prognosis was excellent for patients within the screening programme who were diagnosed with a luminal A‐like primary tumour and/or lymph node metastases. Stage, molecular pathology and mode of detection help to define patients at low risk of death from breast cancer.

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Section: Methodsmentioning

confidence: 99%

Section: Introductionmentioning

confidence: 99%

St Gallen molecular subtypes in screening-detected and symptomatic breast cancer in a prospective cohort with long-term follow-up

Falck

Röme

Fernö

et al. 2016

British Journal of Surgery

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“…Moreover, a larger cohort of breast cancer patients revealed that the luminal subgroup may be divided into luminal A and B 29. Luminal B was previously shown to have a more aggressive phenotype, higher HG, and more proliferative index such as Ki67 than luminal A 30, 31, 32. The prognosis of patients with luminal B tumors was also found to be worse than those with luminal A tumors despite treatments with hormonal therapy 33.…”

Section: Discussionmentioning

confidence: 99%

Prognostic value of the ubiquitin ligase carboxyl terminus of the Hsc70‐interacting protein in postmenopausal breast cancer

et al. 2016

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The carboxyl terminus of the Hsc70‐interacting protein (CHIP) is considered to induce the ubiquitination and degradation of several oncogenic proteins, and play a role in the inhibition of tumor progression and invasion under experimental conditions. However, the impact of CHIP expression on the prognosis of breast cancer patients has not yet been established. In this study, using an immunohistochemical method, 272 patients with invasive breast cancer were assessed for the expression of CHIP (graded scores 0‐3) and the statuses of biomarkers, such as estrogen receptor (ER), progesterone receptor (PgR), and HER2. The relationships between the statuses of CHIP and biomarkers as well as clinical features were also evaluated, and that between the expression of CHIP and patient prognosis was analyzed. We revealed that the strong expression of CHIP correlated with positive ER (P < 0.001), positive PgR (P < 0.001), and negative HER2 (P = 0.02). In postmenopausal patients, relapse‐free survival (RFS) was significantly better in the high CHIP group than in the low CHIP group (P = 0.042). In addition, RFS and cancer‐specific survival (CSS) were significantly better in patients with ER‐positive/CHIP score 3 tumors than in those with ER‐negative/CHIP score 0 tumors (RFS: P = 0.038, CSS: P = 0.0098). The methylation status of CHIP gene promoter did not always account for the down‐regulation of its expression. In conclusion, the overexpression of CHIP is a potent prognostic factor of a good prognosis in ER‐positive breast cancer patients in the postmenopausal phase.

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“…Breast cancer subtypes were defined to histopathological characteristics such as receptor status and grading according to the St. Gallen classification and by von Minckwitz and colleagues (Goldhirsch et al ., 2013; von Minckwitz et al ., 2012). …”

Section: Methodsmentioning

confidence: 99%

TGFβ1 regulates HGF‐induced cell migration and hepatocyte growth factor receptor MET expression via C‐ets‐1 and miR‐128‐3p in basal‐like breast cancer

et al. 2018

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Breast cancer is the most common cancer in women worldwide. The tumor microenvironment contributes to tumor progression by inducing cell dissemination from the primary tumor and metastasis. TGFβ signaling is involved in breast cancer progression and is specifically elevated during metastatic transformation in aggressive breast cancer. In this study, we performed genomewide correlation analysis of TGFBR2 expression in a panel of 51 breast cancer cell lines and identified that MET is coregulated with TGFBR2. This correlation was confirmed at the protein level in breast cancer cell lines and human tumor tissues. Flow cytometric analysis of luminal and basal‐like breast cancer cell lines and examination of 801 tumor specimens from a prospective cohort of breast cancer patients using reverse phase protein arrays revealed that expression of TGFBR2 and MET is increased in basal‐like breast cancer cell lines, as well as in triple‐negative breast cancer tumor tissues, compared to other subtypes. Using real‐time cell analysis technology, we demonstrated that TGFβ1 triggered hepatocyte growth factor (HGF)‐induced and MET‐dependent migration in vitro. Bioinformatic analysis predicted that TGFβ1 induces expression of C‐ets‐1 as a candidate transcription factor regulating MET expression. Indeed, TGFβ1‐induced expression of ETS1 and breast cancer cell migration was blocked by knockdown of ETS1. Further, we identified that MET is a direct target of miR‐128‐3p and that this miRNA is negatively regulated by TGFβ1. Overexpression of miR‐128‐3p reduced MET expression and abrogated HGF‐induced cell migration of invasive breast cancer cells. In conclusion, we have identified that TGFβ1 regulates HGF‐induced and MET‐mediated cell migration, through positive regulation of C‐ets‐1 and negative regulation of miR‐128‐3p expression in basal‐like breast cancer cell lines and in triple‐negative breast cancer tissue.

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Personalizing the treatment of women with early breast cancer: highlights of the St Gallen International Expert Consensus on the Primary Therapy of Early Breast Cancer 2013

Cited by 3,040 publications

References 97 publications

St Gallen molecular subtypes in screening-detected and symptomatic breast cancer in a prospective cohort with long-term follow-up

St Gallen molecular subtypes in screening-detected and symptomatic breast cancer in a prospective cohort with long-term follow-up

Prognostic value of the ubiquitin ligase carboxyl terminus of the Hsc70‐interacting protein in postmenopausal breast cancer

TGFβ1 regulates HGF‐induced cell migration and hepatocyte growth factor receptor MET expression via C‐ets‐1 and miR‐128‐3p in basal‐like breast cancer

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