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Showing content from https://pubmed.ncbi.nlm.nih.gov/16609087/ below:

Estrogen-receptor status and outcomes of modern chemotherapy for patients with node-positive breast cancer

Randomized Controlled Trial

Affiliations

• ¹ University of Texas M. D. Anderson Cancer Center, Houston, TX 77030-4009, USA. rry@mdanderson.org

• PMID: 16609087
• PMCID: PMC1459540
• DOI: 10.1001/jama.295.14.1658

Item in Clipboard

Randomized Controlled Trial

Donald A Berry et al. JAMA. 2006.

• ¹ University of Texas M. D. Anderson Cancer Center, Houston, TX 77030-4009, USA. rry@mdanderson.org

• PMID: 16609087
• PMCID: PMC1459540
• DOI: 10.1001/jama.295.14.1658

Item in Clipboard

• JAMA. 2006 May 24;295(20):2356

Context: Breast cancer estrogen-receptor (ER) status is useful in predicting benefit from endocrine therapy. It may also help predict which patients benefit from advances in adjuvant chemotherapy.

Objective: To compare differences in benefits from adjuvant chemotherapy achieved by patients with ER-negative vs ER-positive tumors.

Design, setting, and patients: Trial data from the Cancer and Leukemia Group B and US Breast Cancer Intergroup analyzed; patient outcomes by ER status compared using hazards over time and multivariate models. Randomized trials comparing (1): 3 regimens of cyclophosphamide, doxorubicin, and fluorouracil (January 1985 to April 1991); (2) 3 doses of doxorubicin concurrent with cyclophosphamide, with or without subsequent paclitaxel (May 1994 to April 1997); (3) sequential doxorubicin, paclitaxel, and cyclophosphamide with concurrent doxorubicin and cyclophosphamide followed by paclitaxel, and also 3-week vs 2-week cycles (September 1997 to March 1999). A total of 6644 node-positive breast cancer patients received adjuvant treatment.

Main outcome measures: Disease-free and overall survival.

Results: For ER-negative tumors, chemotherapy improvements reduced the relative risk of recurrence by 21%, 25%, and 23% in the 3 studies, respectively, and 55% comparing the lowest dose in the first study with biweekly cycles in the third study. Corresponding relative risk reductions for ER-positive tumors treated with tamoxifen were 9%, 12%, and 8% in the 3 studies, and 26% overall. The overall mortality rate reductions associated with chemotherapy improvements were 55% and 23% among ER-negative and ER-positive patients, respectively. All individual ER-negative comparisons and no ER-positive comparisons were statistically significant. Absolute benefits due to chemotherapy were greater for patients with ER-negative compared with ER-positive tumors: 22.8% more ER-negative patients survived to 5 years disease-free if receiving chemotherapy vs 7.0% for ER-positive patients; corresponding improvements for overall survival were 16.7% vs 4.0%.

Conclusion: Among patients with node-positive tumors, ER-negative breast cancer, biweekly doxorubicin/cyclophosphamide plus paclitaxel lowers the rate of recurrence and death by more than 50% in comparison with low-dose cyclophosphamide, doxorubicin, and fluorouracil as used in the first study.

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C…

C denotes cyclophosphamide, A doxorubicin, F fluorouracil, and P paclitaxel. Study 8541 had three treatment arms, with doses of C, A and F in proportion to the dose of doxorubicin that is shown (in milligrams per square meter of body surface area). Study 9344 had a 3 by 2 factorial design, with randomization to one of 3 doses of A with a second randomization to 4 cycles of paclitaxel or not. Study 9741 had a 2 by 2 factorial design, with patients being randomized to biweekly vs triweekly schedules and separately to concurrent AC followed by P vs sequential A followed by P then C.

Cumulative at-risk sample sizes over time are shown in each panel. The initial sample sizes were approximately equally divided among the groups in question. The dose effect of doxorubicin in study 9344 and the comparison of sequential or concurrent therapy in study 9741 are not shown; neither factor was associated with disease-free survival in unadjusted or adjusted analyses, nor were there significant differences within ER subgroups.

Cumulative at-risk sample sizes over time are shown in each panel. The initial sample sizes were approximately equally divided among the groups in question. The dose effect of doxorubicin in study 9344 and the comparison of sequential or concurrent therapy in study 9741 are not shown; neither factor was associated with disease-free survival in unadjusted or adjusted analyses, nor were there significant differences within ER subgroups.

Risk…

Risk was calculated as the number of events during the year divided by the number of patients at risk for experiencing the event at the beginning of the year. Cumulative at-risk sample sizes over time are shown in the respective panels of Figure 2. In the rightmost parts of the curves the samples were relatively small, and the standard errors (not shown) were correspondingly large. Not all patients have reached the later follow-up times. In addition, patients with earlier recurrences have been eliminated from the at-risk group.

Risk…

Risk was calculated as the number of events during the year divided by the number of patients at risk for experiencing the event at the beginning of the year. Cumulative at-risk sample sizes over time are shown in the respective panels of Figure 2. In the rightmost parts of the curves the samples were relatively small, and the standard errors (not shown) were correspondingly large. Not all patients have reached the later follow-up times. In addition, patients with earlier recurrences have been eliminated from the at-risk group.

Panel A shows the risks for patients not receiving tamoxifen (initial n=552), and Panel B shows the risks for patients receiving tamoxifen (same as Panel B of Figure 3) (initial n=472).

Patients have mean tumor size, number of positive lymph nodes and menopausal status as in the low-dose arm of Study 8541. The “Modeled q2wk in Study 9741” curves do not apply to the patients in Study 9741 but instead for patients having the characteristics of the low-dose arm of Study 8541. Both panels A (DFS) and C (OS) show an average reduction in hazard of 55 percent for ER-negative disease while panels B (DFS) and D (OS) show average reductions of 26 and 23 percent for ER-positive disease receiving tamoxifen (see Table 2). The proportional hazards model assumption is that average reduction in hazard applies over the entire 20-year period. The p-values shown are from multivariate models for given ER status. The ER status by chemotherapy interaction p-value for DFS is 0.02 and for OS is 0.05.

• 21-Gene Recurrence Score for prognosis and prediction of taxane benefit after adjuvant chemotherapy plus endocrine therapy: results from NSABP B-28/NRG Oncology.

  Mamounas EP, Tang G, Paik S, Baehner FL, Liu Q, Jeong JH, Kim SR, Butler SM, Jamshidian F, Cherbavaz DB, Sing AP, Shak S, Julian TB, Lembersky BC, Lawrence Wickerham D, Costantino JP, Wolmark N. Mamounas EP, et al. Breast Cancer Res Treat. 2018 Feb;168(1):69-77. doi: 10.1007/s10549-017-4550-8. Epub 2017 Nov 11. Breast Cancer Res Treat. 2018. PMID: 29128898 Free PMC article. Clinical Trial.

• Clinical validation of the EndoPredict test in node-positive, chemotherapy-treated ER+/HER2- breast cancer patients: results from the GEICAM 9906 trial.

  Martin M, Brase JC, Calvo L, Krappmann K, Ruiz-Borrego M, Fisch K, Ruiz A, Weber KE, Munarriz B, Petry C, Rodriguez CA, Kronenwett R, Crespo C, Alba E, Carrasco E, Casas M, Caballero R, Rodriguez-Lescure A. Martin M, et al. Breast Cancer Res. 2014 Apr 12;16(2):R38. doi: 10.1186/bcr3642. Breast Cancer Res. 2014. PMID: 24725534 Free PMC article.

• Adjuvant chemotherapy followed by goserelin versus either modality alone for premenopausal lymph node-negative breast cancer: a randomized trial.

  International Breast Cancer Study Group (IBCSG); Castiglione-Gertsch M, O'Neill A, Price KN, Goldhirsch A, Coates AS, Colleoni M, Nasi ML, Bonetti M, Gelber RD. International Breast Cancer Study Group (IBCSG), et al. J Natl Cancer Inst. 2003 Dec 17;95(24):1833-46. doi: 10.1093/jnci/djg119. J Natl Cancer Inst. 2003. PMID: 14679153 Clinical Trial.

• Adjuvant chemotherapy in early breast cancer.

  Ejlertsen B. Ejlertsen B. Dan Med J. 2016 May;63(5):B5222. Dan Med J. 2016. PMID: 27127018 Review.

• Tamoxifen for early breast cancer. Early Breast Cancer Trialists' Collaborative Group. Early Breast Cancer Trialists' Collaborative Group. Cochrane Database Syst Rev. 2001;(1):CD000486. doi: 10.1002/14651858.CD000486. Cochrane Database Syst Rev. 2001. PMID: 11279694 Updated. Review.

• Value of TP53 status for predicting response to neoadjuvant chemotherapy in breast cancer: a meta-analysis.

  Chen MB, Zhu YQ, Xu JY, Wang LQ, Liu CY, Ji ZY, Lu PH. Chen MB, et al. PLoS One. 2012;7(6):e39655. doi: 10.1371/journal.pone.0039655. Epub 2012 Jun 29. PLoS One. 2012. PMID: 22768103 Free PMC article.

• Systemic cancer therapy: achievements and challenges that lie ahead.

  Palumbo MO, Kavan P, Miller WH Jr, Panasci L, Assouline S, Johnson N, Cohen V, Patenaude F, Pollak M, Jagoe RT, Batist G. Palumbo MO, et al. Front Pharmacol. 2013 May 7;4:57. doi: 10.3389/fphar.2013.00057. eCollection 2013. Front Pharmacol. 2013. PMID: 23675348 Free PMC article.

• Triple-negative breast cancer: role of specific chemotherapy agents.

  Isakoff SJ. Isakoff SJ. Cancer J. 2010 Jan-Feb;16(1):53-61. doi: 10.1097/PPO.0b013e3181d24ff7. Cancer J. 2010. PMID: 20164691 Free PMC article. Review.

• Therapeutic usefulness of postoperative adjuvant chemotherapy with Tegafur-Uracil (UFT) in patients with breast cancer: focus on the results of clinical studies in Japan.

  Nakayama T, Noguchi S. Nakayama T, et al. Oncologist. 2010;15(1):26-36. doi: 10.1634/theoncologist.2009-0255. Epub 2010 Jan 15. Oncologist. 2010. PMID: 20080863 Free PMC article. Review.

• Using clinical trial data to tailor adjuvant treatments for individual patients.

  Regan MM, Gelber RD; International Breast Cancer Study Group (IBCSG) and the Breast International Group (BIG). Regan MM, et al. Breast. 2007 Dec;16 Suppl 2(Suppl 2):S98-104. doi: 10.1016/j.breast.2007.07.016. Epub 2007 Aug 23. Breast. 2007. PMID: 17719227 Free PMC article.

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