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dc.contributor.authorSmith, David B
dc.contributor.authorWagstaff, John
dc.contributor.authorThatcher, Nick
dc.contributor.authorScarffe, J Howard
dc.date.accessioned2010-07-21T09:56:13Z
dc.date.available2010-07-21T09:56:13Z
dc.date.issued1987
dc.identifier.citationA phase I study of rDNA alpha-2b interferon as a 6-week continuous intravenous infusion. 1987, 20 (4):327-31 Cancer Chemother. Pharmacol.en
dc.identifier.issn0344-5704
dc.identifier.pmid3690806
dc.identifier.doi10.1007/BF00262586
dc.identifier.urihttp://hdl.handle.net/10541/108004
dc.description.abstractSixteen patients with advanced malignancy were treated with rDNA alpha-2b interferon using a continuous 6-week i.v. schedule. Patients received 1 microgram, 3 mu [corrected], 5 mu and 7 mu/m2/day via a portable infusion pump system, all therapy being on an outpatient basis. The dose-limiting toxicity occurring at 7 mu/m2/day [corrected] was lethargy and somnolence. Five million units (mu) was the maximum tolerated dose but significant nausea, anorexia and lethargy affected 4/5 patients at this level. A dose of 3 mu/m2/day was well tolerated, producing little disturbance of normal activity in the majority of patients. Suppression of WBC and platelets was seen at all doses but was not dose-limiting. There was increasing severity of derangement of hepatic transaminases with increasing dose, and the occurrence of liver toxicity appeared to correlate with nausea, anorexia and lethargy. Assay of serum interferon during the infusion showed that this system maintained a constant level of interferon in the blood. However, the increase did not show a linear pattern with increasing dose, suggesting saturation of metabolic inactivation at 7 mu/m2/day. We recommend that a dose of 3 mu/m2/day be used in future studies of prolonged infusions of alpha-2 interferon.
dc.language.isoenen
dc.subjectHaematologic Diseasesen
dc.subject.meshAdult
dc.subject.meshAnorexia
dc.subject.meshDrug Evaluation
dc.subject.meshDrug-Induced Liver Injury
dc.subject.meshHematologic Diseases
dc.subject.meshHumans
dc.subject.meshInfusions, Intravenous
dc.subject.meshInterferon Type I
dc.subject.meshMelanoma
dc.subject.meshMiddle Aged
dc.subject.meshMultiple Myeloma
dc.subject.meshNausea
dc.subject.meshRecombinant Proteins
dc.titleA phase I study of rDNA alpha-2b interferon as a 6-week continuous intravenous infusion.en
dc.typeArticleen
dc.contributor.departmentCancer Research Campaign Department of Medical Oncology, Christie Hospital and Holt Radium Institute, Manchester, UK.en
dc.identifier.journalCancer Chemotherapy and Pharmacologyen
html.description.abstractSixteen patients with advanced malignancy were treated with rDNA alpha-2b interferon using a continuous 6-week i.v. schedule. Patients received 1 microgram, 3 mu [corrected], 5 mu and 7 mu/m2/day via a portable infusion pump system, all therapy being on an outpatient basis. The dose-limiting toxicity occurring at 7 mu/m2/day [corrected] was lethargy and somnolence. Five million units (mu) was the maximum tolerated dose but significant nausea, anorexia and lethargy affected 4/5 patients at this level. A dose of 3 mu/m2/day was well tolerated, producing little disturbance of normal activity in the majority of patients. Suppression of WBC and platelets was seen at all doses but was not dose-limiting. There was increasing severity of derangement of hepatic transaminases with increasing dose, and the occurrence of liver toxicity appeared to correlate with nausea, anorexia and lethargy. Assay of serum interferon during the infusion showed that this system maintained a constant level of interferon in the blood. However, the increase did not show a linear pattern with increasing dose, suggesting saturation of metabolic inactivation at 7 mu/m2/day. We recommend that a dose of 3 mu/m2/day be used in future studies of prolonged infusions of alpha-2 interferon.


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