| Literature DB >> 23505515 |
Zsuzsanna Varga1, Peter Sinn, Florian Fritzsche, Arthur von Hochstetter, Aurelia Noske, Peter Schraml, Christoph Tausch, Andreas Trojan, Holger Moch.
Abstract
AIM: Several multigene expression-based tests offering prognostic and predictive information in hormone-receptor positive early breast cancer were established during the last years. These tests provide prognostic information on distant recurrences and can serve as an aid in therapy decisions. We analyzed the recently validated reverse-transcription-quantitative-real-time PCR-based multigene-expression Endopredict (EP)-test on 34 hormone-receptor positive breast-cancer cases and compared the EP scores with the Oncotype DX Recurrence-scores (RS) obtained from the same cancer samples.Entities:
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Year: 2013 PMID: 23505515 PMCID: PMC3591350 DOI: 10.1371/journal.pone.0058483
Source DB: PubMed Journal: PLoS One ISSN: 1932-6203 Impact factor: 3.240
Summary of clinical data.
| n = 34 | ||
| Age (years) | <40 | 3 |
| >40 | 31 | |
| Tumor size | pT1b (0.5 to 1 cm) | 5 |
| pT1c (>1 to 2 cm) | 19 | |
| pT2 (>2 to 5 cm) | 8 | |
| pT3 (>5 cm) | 2 | |
| Nodal status | negative | 21 |
| positive | 13 | |
| Grading | 1 | 2 |
| 2 | 21 | |
| 3 | 11 | |
| ER status | positive | 34 |
| Negative | – | |
| PR status | positive | 31 |
| negative | 3 | |
| HER2 status | negative | 33 |
| positive | 1 | |
ER: estrogen receptors, PR: progesterone receptors, NA: not available.
Comparison of EP score and Recurrence score (RS).
| n = 34 | Recurrence score (RS) (three tiered) | |||
| Low risk | Intermediate risk | High risk | ||
| EP score | Low risk | 9 (26%) | 2 (6%) | 0 (0%) |
| High risk | 6 (18%) | 8 (24%) | 9 (26%) | |
RS in three tiered system.
Comparison of EP score and Recurrence score (RS). RS in two tiered system: low vs. intermediate+high risk.
| n = 34 | Recurrence score (RS) (two tiered) | ||
| Low risk | High+Intermediate risk | ||
| EP score | Low risk | 9 (26%) | 2 (6%) |
| High risk | 6 (18%) | 17 (50%) | |
Figure 1Analytical comparison of Recurrence Score with EndoPredict Score (A) and EPclin Score (B). r = Pearson coefficient.
Comparison of EPclin score and Recurrence score (RS). RS in three tiered system.
| n = 34 | Recurrence score (RS) (three tired) | |||
| Low risk | Intermediate risk | High risk | ||
| EPclin score | Low risk | 11 (32%) | 5 (15%) | 3 (9%) |
| High risk | 4 (11%) | 5 (15%) | 6 (18%) | |
Comparison of EPclin score and Recurrence score (RS). RS in two tiered system: low vs. intermediate+high risk.
| n = 34 | Recurrence score (RS) (two tiered) | ||
| Low risk | High+Intermediate risk | ||
| EPclin score | Low risk | 11 (32%) | 8 (24%) |
| High risk | 4 (12%) | 11 (32%) | |
Figure 2Analytical comparison of continuous Ki67 values with Recurrence Score (A) and EndoPredict Score (B). r = Pearson coefficient.
Comparison of ER/PR/HER2 status with Oncotype DX assay and conventional methodology (Immunohistochemistry and fluorescence in situ hybridization ‘FISH’ testing).
| n = 33 | Oncotype DX testing | ||||
| Conventional metholodogy | positive | negative | equivocal | ||
| ER | positive | 33 (100%) | 33 (100%) | – | – |
| negative | – | – | – | – | |
| PR | positive | 30 (91%) | 26 (79%) | 4 (12%) | – |
| negative | 3 (9%) | 1 (3%) | 2 (6%) | – | |
| HER2 | positive | 1 (3%) | 0 | 1 (3%) | – |
| negative | 32 (97%) | – | 31 (94%) | 1 (3%) | |
| equivocal | – | – | – | – | |
In one case results of Oncotype DX for ER/PR/HER2 status were not available.