Phase I-II study of escalating doses of amifostine combined with high-dose cyclophosphamide

被引:0
|
作者
Michele Ghielmini
Sabine Van der Bosch
Manuela Bosshard
Sandro Pampallona
Luca Gabutti
Hans-Peter Egger
Markus Kiess
Franco Cavalli
Cristiana Sessa
机构
[1] Oncology Institute of Southern Switzerland,
[2] Ospedale San Giovanni,undefined
[3] 6500 Bellinzona,undefined
[4] Switzerland,undefined
[5] ForMed,undefined
[6] Statistics for Medicine,undefined
[7] 1983 Evolene,undefined
[8] Switzerland,undefined
[9] Department of Nephrology,undefined
[10] Ospedale Civico,undefined
[11] 6900 Lugano,undefined
[12] Switzerland,undefined
[13] Essex Chemie AG,undefined
[14] PO Box 2769,undefined
[15] 6002 Luzern,undefined
[16] Switzerland,undefined
[17] Contact address: Istituto Oncologico della Svizzera Italiana,undefined
[18] Ospedale Civico,undefined
[19] 6900 Lugano,undefined
[20] Switzerland,undefined
[21] e-mail: mghielmini@ticino.com,undefined
[22] Tel.: +41-91-8056776,undefined
[23] Fax: +41 91 805 67 80
,undefined
来源
Cancer Chemotherapy and Pharmacology | 2001年 / 47卷
关键词
Amifostine Cyclophosphamide Myeloprotection Nephroprotection Blood stem cells;
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摘要
Purpose: To evaluate the feasibility and clinical effects of increasing doses of amifostine administered four times in 1 day with high-dose (HD) cyclophosphamide (CTX). Methods: A group of 16 patients with a diagnosis of lymphoma were treated with HD-CTX given at a total dose of 7 g/m2 subdivided into four doses, each preceded by increasing doses of amifostine. A group of 12 lymphoma patients previously treated with the same HD-CTX regimen was used as historical controls. Results: The dose of amifostine was escalated in cohorts of three patients each from 4×570 mg/m2 to 4×910 mg/m2 without severe toxic effects. Further patients were treated at the highest dose level. Side effects included a fall in blood pressure (always less than 20% of baseline value), asymptomatic hypocalcemia (from a median value of 2.4 to 1.7 mmol/l) and a decrease in creatinine clearance (from a median value of 102 to 85 ml/min). The parameters of hematotoxicity for patients treated in the study were not significantly different from those of the historical control patients. Conclusions: Amifostine can be given safely at a dose of 910 mg/m2 four times in 1 day in combination with HD-CTX. With this schedule amifostine did not show a myeloprotective effect.
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页码:532 / 536
页数:4
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