TY - JOUR
T1 - Cyclophosphamide dose intensification may circumvent anthracycline resistance of p53 mutant breast cancers
AU - Lehmann-Che, Jacqueline
AU - André, Fabrice
AU - Desmedt, Christine
AU - Mazouni, Chafika
AU - Giacchetti, Sylvie
AU - Turpin, Elisabeth
AU - Espié, Marc
AU - Plassa, Louis François
AU - Marty, Michel
AU - Bertheau, Philippe
AU - Sotiriou, Christos
AU - Piccart, Martine
AU - Symmans, W. Fraser
AU - Pusztai, Lajos
AU - de Thé, Hugues
PY - 2010/1/1
Y1 - 2010/1/1
N2 - The predictive value of p53 for the efficacy of front-line anthracycline-based chemotherapy regimens has been a matter of significant controversy. Anthracyclines are usually combined with widely different doses of alkylating agents, which may significantly modulate tumor response to these combinations. We analyzed three series of de novo stage II-III breast cancer patients treated front line with anthracycline-based regimens of various cyclophosphamide dose intensities: 65 patients with estrogen receptor (ER) tumors treated with anthracyclines alone (Institut Jules Bordet, Brussels), 51 unselected breast cancer patients treated with intermediate doses of cyclophosphamide (MD Anderson Cancer Center, Houston, TX), and 128 others treated with a dose-dense anthracycline-cyclophosphamide combination (St. Louis, Paris). After chemotherapy and surgery, pathologic complete response (pCR) was evaluated. p53 status was determined by a yeast functional assay on the pretreatment tumor sample. In a multivariate analysis of the pooled results, a lack of ER expression and high-dose cyclophosphamide administration were associated with a higher likelihood of pCR. A sharp statistical interaction was detected between p53 status and cyclophosphamide dose intensity. Indeed, when restricting our analysis to patients with ER tumors, we confirmed that a mutant p53 status was associated with anthracycline resistance, but found that p53 inactivation was required for response to the dose-intense alkylating regimen. The latter allowed very high levels of pCR in triple-negative tumors. Thus, our data strongly suggest that cyclophosphamide dose intensification in ER p53-mutated breast cancer patients could significantly improve their response.
AB - The predictive value of p53 for the efficacy of front-line anthracycline-based chemotherapy regimens has been a matter of significant controversy. Anthracyclines are usually combined with widely different doses of alkylating agents, which may significantly modulate tumor response to these combinations. We analyzed three series of de novo stage II-III breast cancer patients treated front line with anthracycline-based regimens of various cyclophosphamide dose intensities: 65 patients with estrogen receptor (ER) tumors treated with anthracyclines alone (Institut Jules Bordet, Brussels), 51 unselected breast cancer patients treated with intermediate doses of cyclophosphamide (MD Anderson Cancer Center, Houston, TX), and 128 others treated with a dose-dense anthracycline-cyclophosphamide combination (St. Louis, Paris). After chemotherapy and surgery, pathologic complete response (pCR) was evaluated. p53 status was determined by a yeast functional assay on the pretreatment tumor sample. In a multivariate analysis of the pooled results, a lack of ER expression and high-dose cyclophosphamide administration were associated with a higher likelihood of pCR. A sharp statistical interaction was detected between p53 status and cyclophosphamide dose intensity. Indeed, when restricting our analysis to patients with ER tumors, we confirmed that a mutant p53 status was associated with anthracycline resistance, but found that p53 inactivation was required for response to the dose-intense alkylating regimen. The latter allowed very high levels of pCR in triple-negative tumors. Thus, our data strongly suggest that cyclophosphamide dose intensification in ER p53-mutated breast cancer patients could significantly improve their response.
UR - http://www.scopus.com/inward/record.url?scp=77950530561&partnerID=8YFLogxK
U2 - 10.1634/theoncologist.2009-0243
DO - 10.1634/theoncologist.2009-0243
M3 - Article
C2 - 20228131
AN - SCOPUS:77950530561
SN - 1083-7159
VL - 15
SP - 246
EP - 252
JO - Oncologist
JF - Oncologist
IS - 3
ER -