Vol. 27, No. 6, 2004
Free Abstract
Article (PDF 104 KB)
Original Article · Originalarbeit
Clinical Phase II Study of Pegylated Liposomal Doxorubicin as Second-Line Treatment in Disseminated Melanoma
W. Finka; C. Zimpfer-Rechnera; A. Thoelkea; R. Figla; M. Kaatzb; M. Ugurela; D. Schadendorfa
aSkin Cancer Unit (German Cancer Research Center) at the Department of Dermatology, University Hospital Mannheim,
bDepartment of Dermatology, University Jena, Germany
Onkologie 2004;27:540-544
(DOI: 10.1159/000081335)
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Summary
Background: Stage IV melanoma has a poor prognosis with
a median survival of 3-11 months from diagnosis of distant
metastases. Response rates in first-line regimens range
around 15-20%. Non-responders have a median survival
around 6 months. Currently, no second-line treatment in advanced
melanoma has been established. Patients and Methods:
In a clinical phase II study we evaluated the efficacy of
liposomal doxorubicin (Caelyx?) in 30 patients (17 m, 13 f)
with progressing metastatic melanoma who had failed a
previous chemotherapy. Liposomal doxorubicin was given
in an outpatient setting at a dose of 50 mg/m2 i.v. on d1,
d22, d43 and d64, subsequently at 40 mg/m2 at d85 before
first staging and in 4-week intervals thereafter. Treatment
was very well tolerated with 100 cycles given in total. Response
rate, survival time, time-to-progression and toxicity
were assessed. Results: Erythrodysesthesia was the most
severe toxicity in 6% at CTC grade 3. Liposomal doxorubicin
was of limited clinical efficacy with 21 patients progressing
within the first 12 weeks. However, 7 patients were treated
3-9 months and were stable for >90 days, achieving 5 SD,
1 PR and 1 CR. Median survival after initiation of second-line
treatment was 214 days (95% CI: 151-304 days) with 7 patients
surviving >300 and 5 patients >400 days. Conclusions:
Liposomal doxorubin as monotherapy is well tolerated but
of limited clinical efficacy. Whether the survival benefit of a
significant proportion of patients (20%) holds true in larger
cohorts and whether the efficacy of liposomal doxorubicin
can be improved by combinations without compromising
the low toxicity profile needs further studies.
Copyright © 2004 S. Karger GmbH, Freiburg
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