Toxicity and effectivity of high-dose idarubicin during AML induction therapy: Results of a pilot study in children

Citation
U. Creutzig et al., Toxicity and effectivity of high-dose idarubicin during AML induction therapy: Results of a pilot study in children, KLIN PADIAT, 212(4), 2000, pp. 163-168
Citations number
17
Categorie Soggetti
Pediatrics
Journal title
KLINISCHE PADIATRIE
ISSN journal
03008630 → ACNP
Volume
212
Issue
4
Year of publication
2000
Pages
163 - 168
Database
ISI
SICI code
0300-8630(200007/08)212:4<163:TAEOHI>2.0.ZU;2-#
Abstract
Background: Idarubicin (IDR) is one of the most effective, but also toxic d rugs in the treatment of AML. The standard dose used in children and adults is 8-12 mg/m(2) during induction. Patients and methods: To improve outcome , we increased the IDR dose from 12 mg/m(2) (standard dose in study AML-BFM 93), applied over three days during induction therapy (AIE = Ara-C, Idarub icin, Etoposide) to 14 mg/m(2) in a pilot study including 17 patients (16 w ith de novo AML, one with secondary AML). Outcome and toxicities were compa red with the other patients of study AML-BFM 93, treated with 3 x 12 mg/m(2 ) IDR or 6 x 30 mg/m(2) daunorubicin (DNR). Results: Patients of the pilot study achieved a good blast cell reduction in the bone marrow on day 15, a high CR rate of 94% and a low relapse rate (3/17 pts.), however, not signif icantly different to the IDR (12 mg/m(2)) group. Hematological toxicity was high, median duration until neutrophil recovery >500/mu l was 25.0 (12-66) days, and similar to the IDR (12 mg/m(2)) and DNR groups. Duration of thro mbocytopenia (time to > 20 000/mu l ) was 21 (10-66) days in the pilot stud y compared to 19 (7-26) days in DNR patients (p = 0.08). four of 17 pilot p atients presented with severe WHO grades 3/4 of mucositis during induction. One patient died in long-lasting aplasia after the 3rd treatment block. Co nclusion: Results of this pilot study show that the IDR 14 mg/m(2) regimen was effective but also toxic. According to our results which, however, are based on small patient numbers, an improved outcome compared to the IDR 12 mg/m(2) regimen seems to be unlikely, therefore the possibly increased toxi city might not be acceptable.