Proposal for classifying the acute emetogenicity of cancer chemotherapy Journal Article

  


Authors: Hesketh, P. J.; Kris, M. G.; Grunberg, S. M.; Beck, T.; Hainsworth, J. D.; Harker, G.; Aapro, M. S.; Gandara, D.; Lindley, C. M.
Article Title: Proposal for classifying the acute emetogenicity of cancer chemotherapy
Abstract: Purpose: To propose a classification of the acute emetogenicity of antineoplastic chemotherapy agents, and to develop an algorithm to define the emetogenicity of combination chemotherapy regimens. Methods: A Medline search was conducted to identify (1) clinical trials that used chemotherapy as single-agent therapy, and (2) major reviews of antiemetic therapy, The search was limited to patients who received commonly used doses of chemotherapy agents, primarily by short(< 3 hours) intravenous infusions. Based on review of this information and our collective clinical experience, we assigned chemotherapy agents to one of five emetogenic levels by consensus. A preliminary algorithm to determine the emetogenicity of combination chemotherapy regimens was then designed by consensus. A final algorithm was developed after we analyzed a data base composed of patients treated on the placebo arms of four randomized antiemetic trials. Results: Chemotherapy agents were divided into five levels: level 1 (< 10% of patients experience acute [less than or equal to 24 hours after chemotherapy] emesis without antiemetic prophylaxis); level 2 (10% to 30%); level 3 (30% to 60%); level 4 (60% to 90%); and level 5 (> 90%). For combinations, the emetogenic level was determined by identifying the most emetogenic agent in the combination and then assessing the relative contribution of the other agents. The following rules apply: (1) level 1 agents do not contribute to the emetogenic level of a combination; (2) adding greater than or equal to one level 2 agent increases the emetogenicity of the combination by one level greater than the most emetogenic agent in the combination; and (3) adding level 3 or 4 agents increases the emetogenicity of the combination by one level per agent. Conclusion: The proposed classification schema provides a practical means to determine the emetogenic potential of individual chemotherapy agents and combination regimens during the 24 hours after administration. This system can serve as a framework for the development of antiemetic guidelines. (C) 1997 by American Society of Clinical Oncology.
Keywords: trial; randomized; phase-ii trial; chronic; non-hodgkins-lymphoma; cell lung-cancer; lymphocytic-leukemia; european-organization; advanced breast-cancer; induced nausea; high-dose cyclophosphamide; oral ondansetron
Journal Title: Journal of Clinical Oncology
Volume: 15
Issue: 1
ISSN: 0732-183X
Publisher: American Society of Clinical Oncology  
Date Published: 1997-01-01
Start Page: 103
End Page: 109
Language: English
ACCESSION: WOS:A1997WB90700015
PROVIDER: wos
PUBMED: 8996130
DOI: 10.1200/JCO.1997.15.1.103
Notes: Article; Proceedings Paper -- Presented in part at the 7th Annual Meeting of the International Association of Supportive Care in Cancer in Luxembourg, Belgium on 1995 Sep 21, 1995 -- Source: Wos
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  1. Mark Kris
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