Dose and Dose Intensity of Adjuvant Chemotherapy for Stage II, Node-Positive Breast Carcinoma

Wood, William C.; Budman, Daniel R.; Korzun, Ann H.; Cooper, M. Robert; Younger, Jerry; Hart, Ronald D.; Moore, Anne; Ellerton, John; Norton, Larry; Ferree, Carolyn; Ballow, Anita Colangelo; Frei, Emil; Henderson, I. Craig

doi:10.1056/nejm199405053301801

Cited by 624 publications

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“…7 Several studies and retrospective analyses suggest a sigDespite adjuvant chemotherapy the prognosis of patients with breast cancer and a high number of nificant dose-response relationship in metastatic and primary breast cancer. [8][9][10][11] Attempts to further improve these involved axillary lymph nodes is very poor. The aim of the present study was to evaluate the efficacy of highresults by increasing the dose of chemotherapy have met only limited success, mainly due to profound myelodose chemotherapy with autologous bone marrow support in patients with seven or more involved axillary suppression.…”

Section: Discussionmentioning

confidence: 99%

High-dose chemotherapy with autologous bone marrow support as consolidation after standard-dose adjuvant therapy in primary breast cancer patients with seven or more involved axillary lymph nodes

Lalisang

Hupperets²,

Haaft³

et al. 1998

Bone Marrow Transplant

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Summary:follow-up data from the CMF Milan experience suggest that even at that time no plateau has been reached. 7 Several studies and retrospective analyses suggest a sigDespite adjuvant chemotherapy the prognosis of patients with breast cancer and a high number of nificant dose-response relationship in metastatic and primary breast cancer. [8][9][10][11] Attempts to further improve these involved axillary lymph nodes is very poor. The aim of the present study was to evaluate the efficacy of highresults by increasing the dose of chemotherapy have met only limited success, mainly due to profound myelodose chemotherapy with autologous bone marrow support in patients with seven or more involved axillary suppression. Autologous bone marrow support (ABMS) offers an opportunity to overcome this problem, but lymph nodes. Nineteen patients underwent four courses of standard adjuvant chemotherapy, followed by highwhether this will lead to better results remains to be determined. dose busulphan/cyclophosphamide chemotherapy with autologous bone marrow support. The median age was High-dose cyclophosphamide has been shown to induce responses in a variety of relapsed or refractory malig-41.4 years and the median number of involved lymph nodes 11. Mucositis WHO grade у3 was observed in nancies and has been part of double alkylator therapy with autologous bone marrow support in advanced breast can-15 patients and 18 patients suffered febrile neutropenia. Transplant-related mortality was encountered in two cer. [12][13][14] Alkylating agents have shown a steep doseresponse relationship in vitro and, when combined, act patients, due to hepatic veno-occlusive disease and sepsis complicated by multi-organ failure, respectively.synergistically to produce response rates higher than those produced by single agents alone. 15,16 After a median follow-up period of 1490 days (range 582-2024 days) from diagnosis, nine patients haveThe preparative regimen busulphan and cyclophosphamide (BuCy) was introduced by Santos and colleagues 17 for relapsed and the overall event-free survival (EFS) is 42% (95% CI 19-65%). The median EFS is 487 days.the treatment of acute non-lymphoblastic leukaemia. This regimen was altered to decrease the toxicity of cyclophosHigh-dose treatment with BuCy2 in high-risk breast cancer patients is a toxic regimen and does not seem to phamide (BuCy2) by Tutschka and coworkers 18 without apparent loss of efficacy. Experience with BuCy2 showed improve disease-free survival. Keywords: adjuvant; bone marrow transplantation; a relatively low treatment-related morbidity, making this bi-alkylator preparative regimen potentially attractive for breast neoplasms drug therapy; busulphan; cyclophosphamide the treatment of solid tumors. 19 In 1991, we started a phase II study to address the question of whether adjuvant chemotherapy followed by highdose consolidation with busulphan and cyclophosphamide Adjuvant chemotherapy has demonstrated a modest, but supported by bone marrow transplantation will improve the consistent improveme...

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Section: Discussionmentioning

confidence: 99%

High-dose chemotherapy with autologous bone marrow support as consolidation after standard-dose adjuvant therapy in primary breast cancer patients with seven or more involved axillary lymph nodes

Lalisang

Hupperets²,

Haaft³

et al. 1998

Bone Marrow Transplant

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“…Only a few controlled prospective studies of the dose-response relationship in breast cancer have been published, and the results have not been consistent. A few studies have demonstrated a survival benefit from receiving a higher dose intensity (Carmo-Pereira et al, 1987;Tannock et al, 1988;Wood et al, 1994), while many controlled studies have failed to demonstrate any dose-response relationship (Hortobagyi et al, 1987a, b;Ludwig Breast Cancer Study Group, 1985;Walters et al, 1992;Fumoleau et al, 1993).…”

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confidence: 99%

Haematological toxicity: a marker of adjuvant chemotherapy efficacy in stage II and III breast cancer

Saarto

Blomqvist²,

Rissanen³

et al. 1997

Br J Cancer

123

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Summary Two hundred and eleven patients with node-positive stage 11 and IlIl breast cancer were treated with eight cycles of adjuvant chemotherapy comprising cyclophosphamide, doxorubicin and oral ftorafur (CAFt), with and without tamoxifen. All patients had undergone radical surgery, and 148 patients were treated with post-operative radiotherapy in two randomized studies. The impact of haematological toxicity of CAFt on distant disease-free (DDFS) and overall survival (OS) was recorded. Dose intensity of all given cycles (Dl), dose intensity of the two initial cycles (Dl2) and total dose (TD) were calculated separately for all chemotherapy drugs and were correlated with DDFS and OS. Patients with a lower leucocyte nadir during the chemotherapy had significantly better DDFS and OS (P = 0.01 and 0.04 respectively). Dose intensity of the two first cycles also correlated significantly with DDFS (P=0.05) in univariate but not in multivariate analysis, while the leucocyte nadir retained its prognostic value. These results indicate that the leucocyte nadir during the adjuvant chemotherapy is a biological marker of chemotherapy efficacy; this presents the possibility of establishing an optimal dose intensity for each patient. The initial dose intensity of adjuvant chemotherapy also seems to be important in assuring the optimal effect of adjuvant chemotherapy.

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“…Recently, Goldhirsch et al concluded that the many variations in CMF regimens did not improve results (Goldhirsch et al, 1998a(Goldhirsch et al, , 1998b. However, several studies have suggested that a higher dose or dose intensity of chemotherapy may improve disease-free and overall survival (Bonadonna and Valagussa, 1981;Hryniuk and Bush, 1984;Hryniuk and Levine, 1986;Hryniuk et al, 1987;Tannock et al, 1988;Ang et al, 1989;Engelsman et al, 1991;Wood et al, 1994). Bonadonna and Valagussa (1981) suggested after a retrospective analysis, that the effectiveness of adjuvant CMF depends on the total dose actually administered.…”

Section: Discussionmentioning

confidence: 99%

“…CMF was only useful when given ≥ 85% of the planned dose (Bonadonna and Valagussa, 1981). Wood et al reported the results of a prospective, randomized trial of adjuvant cyclophosphamide, doxorubicin and 5-fluorouracil in three dose levels (Wood et al, 1994). The women treated with a moderate or high dose intensity had a significantly longer disease-free and overall survival than those treated with a low dose intensity.…”

Section: Discussionmentioning

confidence: 99%

“…Several trials have suggested that relapse-free survival and overall survival not only depend on the total dose of the cytotoxic drugs actually administered, but the more so on the dose intensity, i.e. the amount of drug given per unit of time (Bonadonna and Valagussa, 1981;Hryniuk and Bush, 1984;Hryniuk and Levine, 1986;Hryniuk et al, 1987;Tannock et al, 1988;Ang et al, 1989;Engelsman et al, 1991;Wood et al, 1994).…”

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Summary Our aim was to study the feasibility of an intensified intravenous CMF (cyclophosphamide, methotrexate and 5-fluorouracil) schedule with the aim to escalate dose intensity (DI). Twenty-three premenopausal breast cancer patients received 6 cycles of adjuvant CMF intravenously on days 1 and 8 every 3 weeks and granulocyte colony-stimulating factor days 9-18. Endpoints were DI and toxicity. Twentyone out of 23 patients (91%) received the projected total dose and reached ≥ 85% of the projected DI. Compared to 'classical' CMF, all patients reached ≥ 111% DI. Nine patients received the planned schedule without delay. Thirteen patients (57%) were treated for infection and four patients (17%) were hospitalized for febrile neutropenia. Twelve patients received red blood cell transfusions (52%). Radiation therapy (n = 6) had no adverse impact on dose intensity or haematological toxicity. This dose-intensified CMF schedule was accompanied by enhanced haematological toxicity with clinical sequelae, namely fever, intravenous antibiotics and red blood cell transfusions, but allows a high dose intensity in a majority of patients.

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Dose and Dose Intensity of Adjuvant Chemotherapy for Stage II, Node-Positive Breast Carcinoma

Abstract: The doses of chemotherapy used to treat breast cancer, especially early breast cancer, should not be reduced if the maximal benefit is to be achieved.

Cited by 624 publications

References 13 publications

High-dose chemotherapy with autologous bone marrow support as consolidation after standard-dose adjuvant therapy in primary breast cancer patients with seven or more involved axillary lymph nodes

High-dose chemotherapy with autologous bone marrow support as consolidation after standard-dose adjuvant therapy in primary breast cancer patients with seven or more involved axillary lymph nodes

Haematological toxicity: a marker of adjuvant chemotherapy efficacy in stage II and III breast cancer

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