We read with interest the article by Khaleel and colleagues reporting a new prognostic signature in hormone receptor (HR)-positive breast cancer based on mRNA expression of target genes of the E2F4 transcription factor [1]. The clinical relevance comes from its independent prognostic value and its biological significance (mainly regulation of cell cycle and proliferation, reflecting high E2F4 activity). When compared with patients with low score for the signature (low risk), patients with high score (high risk) showed shorter relapse-free survival, making them candidates for adjuvant chemotherapy. Whereas adjuvant chemotherapy is recommended for most human epidermal growth factor receptor 2 (HER2)-positive or triple-negative tumors, indications are more challenging for HR+/HER2− tumors, which are candidates for either adjuvant hormone therapy alone or both hormone therapy and chemotherapy.
We wondered whether high-risk HR+/HER2− tumors were more chemosensitive than low-risk HR+/HER2− tumors. We gathered gene expression data for 1,247 breast cancers treated with neoadjuvant anthracycline-based chemotherapy and with available pathological response (Additional file 1), pathological complete response (pCR) being defined as no residual invasive cancer in the breast and axillary lymph nodes. All cases were assigned a relapse risk according to the metagene based on average expression of 199 E2F4 target genes in each standardized dataset. We analyzed the predictive value of the E2F4 metagene for the pathological response to chemotherapy in the 582 HR+/HER2− tumors (12% pCR rate). High-risk tumors were associated (Additional file 2) with ductal type, grade 3, and higher pCR rate, which was 17% versus 8% in the low-risk tumors (P <0.001). As expected, grade 3 was also associated with higher pCR rate (Table 1). In multivariate analysis, the E2F4 metagene remained predictive for pCR (P = 0.027), whereas grade did not. Interestingly, mRNA expression of E2F4 itself did not predict for the response to chemotherapy, demonstrating the interest of the metagene as a better indicator of E2F4 function than E2F4 expression level alone.
Table 1.
Univariate analysis | Multivariate analysis | |||||
---|---|---|---|---|---|---|
n | Odds ratio (95% CI) | P value | n | Odds ratio (95% CI) | P value | |
Age, >50 years versus ≤50 years | 582 | 0.79 (0.51 to 1.21) | 0.37 | |||
Histological type | ||||||
ILC versus IDC | 240 | 2.60 (0.71 to 8.12) | 0.19 | |||
Other versus IDC | 1.09 (0.49 to 2.26) | 0.85 | ||||
Clinical tumor size, cT2 to cT4 versus cT1 | 580 | 0.88 (0.44 to 2.01) | 0.79 | |||
Clinical axillary lymph node status, cN1 to cN3 versus cN0 | 571 | 1.37 (0.86 to 2.23) | 0.27 | |||
Grade | ||||||
2 versus 1 | 529 | 1.32 (0.43 to 5.98) | 0.72 | 529 | 1.22 (0.40 to 5.52) | 0.80 |
3 versus 1 | 5.56 (1.93 to 24.4) | 2.09E-02 | 4.37 (1.48 to 19.4) | 0.05 | ||
E2F4 metagene-based classification, high risk versus low risk | 582 | 2.40 (1.57 to 3.72) | 7.98E-04 | 529 | 1.86 (1.14 to 3.08) | 4.02E-02 |
CI, confidence interval; IDC, invasive ductal cancer; ILC, invasive lobular cancer. Bold data indicate significance.
HR+/HER2− tumors with an E2F4 high-risk signature were more sensitive to anthracycline-based chemotherapy than low-risk tumors, as already reported with other prognostic signatures [2,3] – including in the adjuvant setting [4,5], where high-risk tumors showed greater benefit from chemotherapy than low-risk tumors. The next step will be to test, retrospectively in randomized prospective trials of adjuvant chemotherapy, the hypothesis that the difference in relapse between patients treated with chemotherapy and untreated patients is larger in the high-risk group than in the low-risk group. Interest in the E2F4 signature is probably higher than expected.
Acknowledgements
This work is supported by Institut Paoli-Calmettes, Inserm, Institut National du Cancer (AOPL2010 IVOIRES), Ligue Nationale contre le Cancer (label DB) and SIRIC INCa-DGOS-Inserm 6038.
Abbreviations
- HER2
Human epidermal growth factor receptor 2
- HR
Hormone receptor
- pCR
Pathological complete response
Additional files
Footnotes
See related research by Khaleel et al., http://breast-cancer-research.com/content/16/6/486
Competing interests
The authors declare that they have no competing interests.
Authors’ contributions
FB designed the study. FB and PF performed the analyses. FB wrote the manuscript. PF and DB revised the manuscript. All authors approved submission of the manuscript.
Contributor Information
François Bertucci, Email: bertuccif@ipc.unicancer.fr.
Pascal Finetti, Email: bertuccif@ipc.unicancer.fr.
Daniel Birnbaum, Email: bertuccif@ipc.unicancer.fr.
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