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dc.contributor.authorRadford, John A
dc.contributor.authorRyder, W David J
dc.contributor.authorDodwell, David J
dc.contributor.authorAnderson, Heather
dc.contributor.authorThatcher, Nick
dc.date.accessioned2010-07-15T09:12:03Z
dc.date.available2010-07-15T09:12:03Z
dc.date.issued1992
dc.identifier.citationPredicting septic complications of chemotherapy: an analysis of 382 patients treated for small cell lung cancer without dose reduction after major sepsis. 1992, 29A (1):81-6 Eur J Canceren
dc.identifier.issn0959-8049
dc.identifier.pmid1332739
dc.identifier.urihttp://hdl.handle.net/10541/107713
dc.description.abstractThe incidence and risk of septic complications in 382 patients treated for small cell lung cancer with combination chemotherapy at a single centre have been analysed. Full protocol doses were employed throughout with no dose reduction after episodes of severe or life-threatening sepsis (SLTS). 50 (13%) patients experienced 66 episodes of SLTS associated with 1978 cycles of chemotherapy (3.2% cycles affected). 20 (5.2%) patients died due to sepsis (SD) of whom only 4 had experienced SLTS with a previous cycle of treatment. The others died as a result of their first septic episode. A model comprising four variables, age (< or = 50 or > 50 years), Karnofsky performance status (KP < or = 50 or > 50), treatment (two- or three-drug regimen) and previous sepsis (SLTS or no SLTS with previous cycles) was found to satisfactorily describe the incidence of SLTS and SD in the study population and once validated in another patient groups this model should allow identification of high-risk individuals before treatment starts. If so, we propose that high-risk patients (age > 50 years, KP < or = 50, treatment with three-drug regimen) receive 50% of protocol doses in the first cycle of treatment with escalation to 75% and eventually 100% doses in subsequent cycles if sepsis does not supervene. Those with one or two risk factors present run a relatively low risk of SLTS or SD and we consider that full-dose chemotherapy should be used throughout in these individuals.
dc.language.isoenen
dc.subjectLung Canceren
dc.subject.meshAge Factors
dc.subject.meshAntineoplastic Combined Chemotherapy Protocols
dc.subject.meshBacterial Infections
dc.subject.meshCarcinoma, Small Cell
dc.subject.meshHumans
dc.subject.meshImmunocompromised Host
dc.subject.meshIncidence
dc.subject.meshInfection
dc.subject.meshLung Neoplasms
dc.subject.meshMiddle Aged
dc.subject.meshModels, Theoretical
dc.subject.meshPrognosis
dc.subject.meshRisk Factors
dc.subject.meshTime Factors
dc.titlePredicting septic complications of chemotherapy: an analysis of 382 patients treated for small cell lung cancer without dose reduction after major sepsis.en
dc.typeArticleen
dc.contributor.departmentCRC Department of Medical Oncology, Christie Hospital, Manchester, U.K.en
dc.identifier.journalEuropean Journal of Canceren
html.description.abstractThe incidence and risk of septic complications in 382 patients treated for small cell lung cancer with combination chemotherapy at a single centre have been analysed. Full protocol doses were employed throughout with no dose reduction after episodes of severe or life-threatening sepsis (SLTS). 50 (13%) patients experienced 66 episodes of SLTS associated with 1978 cycles of chemotherapy (3.2% cycles affected). 20 (5.2%) patients died due to sepsis (SD) of whom only 4 had experienced SLTS with a previous cycle of treatment. The others died as a result of their first septic episode. A model comprising four variables, age (< or = 50 or > 50 years), Karnofsky performance status (KP < or = 50 or > 50), treatment (two- or three-drug regimen) and previous sepsis (SLTS or no SLTS with previous cycles) was found to satisfactorily describe the incidence of SLTS and SD in the study population and once validated in another patient groups this model should allow identification of high-risk individuals before treatment starts. If so, we propose that high-risk patients (age > 50 years, KP < or = 50, treatment with three-drug regimen) receive 50% of protocol doses in the first cycle of treatment with escalation to 75% and eventually 100% doses in subsequent cycles if sepsis does not supervene. Those with one or two risk factors present run a relatively low risk of SLTS or SD and we consider that full-dose chemotherapy should be used throughout in these individuals.


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