4'Epioxorubicin (Epirubicin): Activity in hepatocellular carcinoma

H. S. Hochster; M. D. Green; J. Speyer

doi:10.1200/JCO.1985.3.11.1535

4'Epioxorubicin (Epirubicin): Activity in hepatocellular carcinoma

H. S. Hochster, M. D. Green, J. Speyer

Research output: Contribution to journal › Article › peer-review

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Abstract

Doxorubicin provides the most consistent response rate inn hepatocellular carcinoma. We therefore initiated a trial with its analog 4'epidoxorubicin. Eighteen patients, all without prior treatment, were given the drug as a single agent every 3 weeks with dose escalation whenever possible. Five patients were treated by six-hour infusion and 13 by intravenous (IV) bolus injection, with the median dose being 90 mg/m². The patients were of diverse ethnic background and included some with underlying cirrhosis and hepatitis B surface antigenemia. Three patients had partial remissions (6, 12, 48 weeks) for a response rate of 17%. Four patients also had prolonged stable disease (14, 26, 27, 38 weeks). Toxicity was mild, although cardiac toxicity developed in three patients at 685, 825, and 1,460 mg/m² cumulative dose. The response to 4'epidoxorubicin in this study appears to be equivalent to the reported response rates for doxorubicin, with decreased toxicity.

Original language	English (US)
Pages (from-to)	1535-1540
Number of pages	6
Journal	Journal of Clinical Oncology
Volume	3
Issue number	11
DOIs	https://doi.org/10.1200/JCO.1985.3.11.1535
State	Published - 1985
Externally published	Yes

All Science Journal Classification (ASJC) codes

Oncology
Cancer Research

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10.1200/JCO.1985.3.11.1535

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title = "4'Epioxorubicin (Epirubicin): Activity in hepatocellular carcinoma",

abstract = "Doxorubicin provides the most consistent response rate inn hepatocellular carcinoma. We therefore initiated a trial with its analog 4'epidoxorubicin. Eighteen patients, all without prior treatment, were given the drug as a single agent every 3 weeks with dose escalation whenever possible. Five patients were treated by six-hour infusion and 13 by intravenous (IV) bolus injection, with the median dose being 90 mg/m2. The patients were of diverse ethnic background and included some with underlying cirrhosis and hepatitis B surface antigenemia. Three patients had partial remissions (6, 12, 48 weeks) for a response rate of 17%. Four patients also had prolonged stable disease (14, 26, 27, 38 weeks). Toxicity was mild, although cardiac toxicity developed in three patients at 685, 825, and 1,460 mg/m2 cumulative dose. The response to 4'epidoxorubicin in this study appears to be equivalent to the reported response rates for doxorubicin, with decreased toxicity.",

author = "Hochster, {H. S.} and Green, {M. D.} and J. Speyer",

year = "1985",

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T1 - 4'Epioxorubicin (Epirubicin)

T2 - Activity in hepatocellular carcinoma

AU - Hochster, H. S.

AU - Green, M. D.

AU - Speyer, J.

PY - 1985

Y1 - 1985

N2 - Doxorubicin provides the most consistent response rate inn hepatocellular carcinoma. We therefore initiated a trial with its analog 4'epidoxorubicin. Eighteen patients, all without prior treatment, were given the drug as a single agent every 3 weeks with dose escalation whenever possible. Five patients were treated by six-hour infusion and 13 by intravenous (IV) bolus injection, with the median dose being 90 mg/m2. The patients were of diverse ethnic background and included some with underlying cirrhosis and hepatitis B surface antigenemia. Three patients had partial remissions (6, 12, 48 weeks) for a response rate of 17%. Four patients also had prolonged stable disease (14, 26, 27, 38 weeks). Toxicity was mild, although cardiac toxicity developed in three patients at 685, 825, and 1,460 mg/m2 cumulative dose. The response to 4'epidoxorubicin in this study appears to be equivalent to the reported response rates for doxorubicin, with decreased toxicity.

AB - Doxorubicin provides the most consistent response rate inn hepatocellular carcinoma. We therefore initiated a trial with its analog 4'epidoxorubicin. Eighteen patients, all without prior treatment, were given the drug as a single agent every 3 weeks with dose escalation whenever possible. Five patients were treated by six-hour infusion and 13 by intravenous (IV) bolus injection, with the median dose being 90 mg/m2. The patients were of diverse ethnic background and included some with underlying cirrhosis and hepatitis B surface antigenemia. Three patients had partial remissions (6, 12, 48 weeks) for a response rate of 17%. Four patients also had prolonged stable disease (14, 26, 27, 38 weeks). Toxicity was mild, although cardiac toxicity developed in three patients at 685, 825, and 1,460 mg/m2 cumulative dose. The response to 4'epidoxorubicin in this study appears to be equivalent to the reported response rates for doxorubicin, with decreased toxicity.

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4'Epioxorubicin (Epirubicin): Activity in hepatocellular carcinoma

Abstract

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