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58. Relationship between hormonal status and clinical response in human fibrocystic disease

Fraioli, F. ; Lavecchia, V. ; Vita, F. ; [et al.]

Amsterdam : Elsevier

Journal of Steroid Biochemistry 11 (1979), S. xxx

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ISSN: 0022-4731

Source: Elsevier Journal Backfiles on ScienceDirect 1907 - 2002

Topics: Biology , Chemistry and Pharmacology

Type of Medium: Electronic Resource

URL: http://linkinghub.elsevier.com/retrieve/pii/0022-4731(79)90422-9

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Oxaliplatin and raltitrexed combined with leucovorin-modulated 5-fluorouracil i.v. bolus every two weeks: A dose finding study in advanced previously treated colorectal carcinoma (2000)

Comella, P. ; De Vita, F. ; De Lucia, L. ; [et al.]

Springer

Annals of oncology 11 (2000), S. 461-468

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ISSN: 1569-8041

Keywords: colorectal carcinoma ; dose-finding study ; modulated 5-fluorouracil ; oxaliplatin ; raltitrexed ; triplet combination

Source: Springer Online Journal Archives 1860-2000

Topics: Medicine

Notes: Abstract Purpose:To determine the maximum tolerated dose of oxaliplatin(L-OHP) given as a two-hour infusion followed by raltitrexed (Tomudex®[TOM]) administered as a 15-min infusion on day 1, and bolus 5-fluorouracil(5-FU) modulated by a fixed dose of levo-folinic acid (LFA) 250mg/m2 on day 2, recycling every two weeks, and to have preliminaryevidence of activity of this combination in pretreated advanced colorectalcancer patients. Patients and methods:Fifty-two patients with advanced colorectalcarcinoma previously treated with one (25 cases) or two or more lines ofchemotherapy, including irinotecan (26 cases), and/or modulated 5-FU (40cases) entered this study. Starting doses of L-OHP, TOM, and 5-FU were 85, 2.5and 750 mg/m2, respectively. Results:Seven dose levels were tested. Neutropenia was the maindose limiting toxicity of the dose escalation (8 of 13 cases). The recommendeddoses were 130 mg/m2 of L-OHP, and 3.0 mg/m2 of TOM onday 1, followed by 250 mg/ m2 of LFA, and 1050 mg/m2 of5-FU on day 2, every two weeks. Severe diarrhoea and stomatitis were rarelyreported. Most patients complained of mild peripheral sensitive neurotoxicity,which was related to the cumulative dose of L-OHP. Twelve patients wereconsidered as having a major responses (one complete), and an additional eightpatients showed a minor response; the median time to treatment failure wastwenty-four weeks. Conclusions:With this regimen it is possible to give full dosesof all three cytotoxic drugs every two weeks. Its activity and its manageabletoxicity profile deserve further evaluation in pretreated advanced colorectalcancer patients.

Type of Medium: Electronic Resource

URL: http://dx.doi.org/10.1023/A:1008308609978

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Concurrent irinotecan and 5-fluorouracil plus levo-folinic acid given every other week in the first-line management of advanced colorectal carcinoma: A phase I study of the Southern Italy Cooperative Oncology Group (1999)

Comella, P. ; Casaretti, R. ; De Vita, F. ; [et al.]

Springer

Annals of oncology 10 (1999), S. 915-921

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ISSN: 1569-8041

Keywords: advanced colorectal carcinoma ; biweekly regimen ; combination chemotherapy ; CPT-11 ; first-line treatment ; 5-fluorouracil, irinotecan

Source: Springer Online Journal Archives 1860-2000

Topics: Medicine

Notes: Abstract Objectives: To determine the maximum tolerable doses (MTDs) of irinotecan (CPT-11) and 5-fluorouracil (5-FU) plus levo-folinic acid (LFA) administered together every two weeks, to define the toxicity profile of this regimen, and to have a preliminary evidence of its activity in the first-line management of advanced colorectal cancer patients. Patients and methods: Patients with histologically proven colorectal carcinoma, no prior chemotherapy for their advanced disease, and with at least one measurable or evaluable indicator lesion, were admitted to this study. The starting dose of CPT-11 was 150 mg/m2 given i.v. (90 min infusion) on day 1, followed on day 2 by a fixed dose of LFA (250 mg/m2) as a two-hour i.v. infusion plus a starting dose of 5-FU 600 mg/m2 as i.v. bolus. No intra-patient dose escalation was allowed. If no dose limiting toxicity (DLT) was observed among three patients of each cohort, CPT-11 and 5-FU were alternately escalated in the subsequent cohort. Otherwise, three more patients were enrolled at the same dose level. DLT was defined as: WHO grade 3 non-haematological toxicity (except for vomiting or alopecia), grade 3 febrile neutropenia, grade 4 neutro- or thombocytopenia, or a 〉2-week delay in recycling. The MTDs were defined as the doses at which two of three, or four of six, patients showed the same DLT. Results: Thirty-one patients (five pretreated in adjuvant setting) were enrolled in this study, and a total number of 293 cycles (median 6/patient) were administered. Dose escalation safely proceeded to 210/950/250 mg/m2 of CPT-11/5-FU/LFA. These dosages were considered as MTDs, since four of six patients showed grade 4 neutropenia, in one case associated with grade 3 stomatitis. A mild decrease of both the CPT-11 and 5-FU doses to 200 and 850 mg/m2, respectively, caused different DLTs (neutropenia and diarrhoea) in two out of seven patients. At these dosages, transient grades 3 or 4 neutropenia affected two patients each during their treatment, while only one patient suffered from a severe delayed diarrhoea. Other non-haematological toxicities were mild and manageable. Therefore, we recommend this latter dose level for further study. Major responses (3 complete and 11 partial) were reported in 14 patients, for an overall response rate of 45% (95% CI: 27%–64%) according to an intent-to-treat analysis. Responses were observed from first dose level, and in four of five previously treated patients. Median failure-free and overall survivals, after a median follow-up of 39 weeks, were 42 and 55 weeks, respectively. Conclusions: The concurrent administration of CPT-11 and modulated 5-FU every two weeks is feasible at the recommended dosages. This regimen demonstrated interesting activity in the management of advanced colorectal cancer patients, and it probably better exploits the synergism between CPT-11 and 5-FU than recently tested alternating schedules. A phase II study is ongoing to more precisely define its activity and toxicity.

Type of Medium: Electronic Resource

URL: http://dx.doi.org/10.1023/A:1008339010655

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Biweekly irinotecan or raltitrexed plus 6S-leucovorin and bolus 5-fluorouracil in advanced colorectal carcinoma: A Southern Italy Cooperative Oncology Group phase II–III randomized trial (2000)

Comella, P. ; De Vita, F. ; Mancarella, S. ; [et al.]

Springer

Annals of oncology 11 (2000), S. 1323-1333

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ISSN: 1569-8041

Keywords: CPT-11 + LFA–5-FU ; colorectal cancer ; phase II–III study ; TOM + LFA–5-FU

Source: Springer Online Journal Archives 1860-2000

Topics: Medicine

Notes: Abstract Purpose:The aim of this randomised trial was to evaluate theactivity and toxicity of a biweekly regimen including 6S-leucovorin-modulated5-fluorouracil (LFA–5-FU), combined with either irinotecan (CPT-11 +LFA–5-FU) or raltitrexed (Tomudex®) (TOM + LFA–5-FU), inadvanced colorectal cancer patients, and to make a preliminary comparison ofboth these experimental regimens with a biweekly administration ofLFA–5-FU modulated by methotrexate (MTX + LFA–5-FU). Patients and methods:One hundred fifty-nine patients withadvanced colorectal carcinoma previously untreated for the metastatic disease(34 of them previously exposed to adjuvant 5-FU) were randomly allocated toreceive: CPT-11, 200 mg/m2 i.v. on day 1, followed on day 2 by LFA,250 mg/m2 i.v. infusion and 5-FU, 850 mg/m2 s i.v. bolus(arm A); TOM, 3 mg/m2 i.v. on day 1, followed on day 2 by LFA, 250mg/m2 i.v. infusion and 5-FU, 1050 mg/m2 i.v. bolus (armB); or MTX, 750 mg/m2 i.v. on day 1, followed on day 2 by LFA, 250mg/m2 i.v. infusion and 5-FU, 800 mg/m2 i.v. bolus (armC). Courses were repeated every two weeks in all arms of the trial. Responserate (RR) was evaluated after every four courses. The sample size was definedto have an 80% power to detect a 35% RR for each experimentaltreatment, and to show a difference of at least 4% in RR with thestandard treatment if the true difference is 15% or more. Results:The RRs were: 34% (95% confidence interval(95% CI): 21%–48%) in arm A, including 3 completeresponses (CRs) and 15 partial responses (PRs), 24% (95% CI:14%–38%) in arm B, including 2 CRs and 11 PRs, and24% (95% CI: 14%–38%), with 2 CRs and 11PRs, in arm C. After a median follow-up time of 62 (range 18–108) weeks,the median time to progression was 38, 25, and 27 weeks for arm A, B, and C,respectively. With 94 patients still alive, the one-year probability ofsurvival was 61%, 54%, and 59%, respectively. WHO grade3 or 4 neutropenia and diarrhoea affected 46% and 16%,respectively, of patients treated with CPT-11 + LFA–5-FU. Medianrelative dose intensity over eight cycles (DI8) was 78% forCPT-11 and 82% for 5-FU. Severe toxicities of TOM + LFA–5-FU wereneutropenia (16%) and diarrhoea (16%), but median relativeDI8 was 93% for TOM, and 82% for 5-FU. Conclusions:CPT-11 + LFA–5-FU compares favorably in termof activity and toxicity with other combination regimens including CPT-11 andcontinuous infusional 5-FU. The hypothesis of a RR 15% higher than theMTX + LFA–5-FU treatment can not be ruled out after this interimanalysis. The TOM + LFA–5-FU regimen showed a RR and a toxicity profilevery close to the MTX + LFA–5-FU combination, and dose not deservefurther evaluation in advanced colorectal cancer patients.

Type of Medium: Electronic Resource

URL: http://dx.doi.org/10.1023/A:1008375705484

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