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1

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The Family System Test (FAST) (1998)

Real del Sartre, O. ; Stiefel, F. ; Leyvraz, S. ; [et al.]

Springer

Supportive care in cancer 6 (1998), S. 416-420

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ISSN: 1433-7339

Keywords: Key words Cancer ; Family constructs ; Family System Test (FAST) ; Psychooncology

Source: Springer Online Journal Archives 1860-2000

Topics: Medicine

Notes: Abstract The impact of a cancer diagnosis upon a family has become a focus of clinical interest, but few scientific studies have been completed in this area. The objectives of this pilot study were twofold: first, to test the applicability of the Family System Test (FAST) in families (n=5) with a young adult member with cancer and secondly to evaluate patterns of interactions within these families. Results show that the FAST is applicable and useful to evaluate the different perceptions of hierarchy and cohesion - two essential variables - within these families. The great majority of family members represented their relationships as balanced (i.e., cohesive and moderately hierarchical). However, contrary to nonclinical families, fathers had a less positive view than mothers and patients: fathers more often perceived family and parenteral relations as unbalanced, and also more often perceived a reversal of hierarchy and a cross-generational coalition within the family. Implications for future research and clinical care are discussed.

Type of Medium: Electronic Resource

URL: http://dx.doi.org/10.1007/s005200050186

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The impact of adding low-dose leucovorin to monthly 5-fluorouracil in advanced colorectal carcinoma: Results of a phase III trial (1998)

Borner, M. M. ; Castiglione, M. ; Bacchi, M. ; [et al.]

Springer

Annals of oncology 9 (1998), S. 535-541

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ISSN: 1569-8041

Keywords: colorectal cancer ; fluorouracil ; low-dose leucovorin ; phase III trial ; survival benefit

Source: Springer Online Journal Archives 1860-2000

Topics: Medicine

Notes: Abstract Purpose: A wide variety of fluorouracil (FU)-plus-leucovorin (LV) doseschedules are in clinical use for the treatment of advanced colorectalcancer. Only the monthly low-dose LV- plus-FU regimen, as used by the NorthCentral Cancer Treatment Group, has demonstrated a lasting survival benefitas opposed to FU alone (J Clin Oncol 1989; 7: 1407–1417). The SwissCancer Group adopted this regimen for a confirmatory phase III trial butused the same dose-intensity of fluorouracil in both treatment arms. Patients and methods: Patients with inoperable or metastatic colorectalcancer were randomized to receive monthly FU 400 mg/m2/dayplus LV 20 mg/m2/day as intravenous push daily for five days,or FU alone. Results: Three hundred nine of the 310 patients randomized were eligibleand included in the analysis. The objective response rate for patients withmeasurable disease was 9% with FU alone and 22% withFU-plus-LV (P = 0.0001). The median progression-free survival was 3.9 versus6.2 months (P = 0.003) and the overall survival 10 versus 12.4 months (P =0.02). The major prognostic factors for survival were performance status,weight loss, and disease symptoms. WHO 〉2 toxicity, consisting ofstomatitis (P = 0.001), diarrhea (P = 0.001), and nausea (P = 0.001), wasmore pronounced for FU-plus-LV, without fatal events. Conclusions: This is the largest published randomized trial to compareFU-plus-LV to FU alone in advanced colorectal cancer. It confirms the survivalbenefit obtained from biomodulating monthly FU with low-dose LV. The toxiceffects of FU-plus-LV were acceptable to most patients, and they respondedwell to FU dose reductions. In the absence of an ideal dose-intense FUmonotherapy regimen, monthly FU with low-dose LV provides a simple andeconomical means by which to achieve adequate FU efficacy in the treatment ofadvanced colorectal cancer.

Type of Medium: Electronic Resource

URL: http://dx.doi.org/10.1023/A:1008270916325

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3

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Cost comparison between PAV and ICE treatment with peripheral blood progenitor cells (PBPC) reinfusion in small-cell lung cancer (SCLC) (1999)

Wasserfallen, J.-B. ; Rollier, P. ; Leyvraz, S. ; [et al.]

Springer

Annals of oncology 10 (1999), S. 243-244

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ISSN: 1569-8041

Source: Springer Online Journal Archives 1860-2000

Topics: Medicine

Type of Medium: Electronic Resource

URL: http://dx.doi.org/10.1023/A:1008308115848

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4

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Saturable metabolism of continuous high-dose ifosfamide with Mesna and GM-CSF: A pharmacokinetic study in advanced sarcoma patients (1999)

Cerny, T. ; Leyvraz, S. ; von Briel, T. ; [et al.]

Springer

Annals of oncology 10 (1999), S. 1087-1094

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ISSN: 1569-8041

Keywords: high-dose ifosfamide ; metabolism ; pharmacology ; sarcomas

Source: Springer Online Journal Archives 1860-2000

Topics: Medicine

Notes: Abstract Background: The aim of this study was to assess the pharmacology, toxicity and activity of high-dose ifosfamide/mesna ± GM-CSF administered by a five-day continuous infusion at a total ifosfamide dose of 12–18 g/m2 in adult patients with advanced sarcomas. Patients and methods: Between January 1991 and October 1992 32 patients with advanced or metastatic sarcoma were entered the study. Twenty-seven patients were pretreated including twenty-three with prior ifosfamide at less than 8 g/m2 total dose/cycle. In 25 patients (27 cycles) extensive pharmacokinetic analyses were performed. Results: The area under the plasma concentration-time curve (AUC) for ifosfamide increased linearly with dose while the AUC's of the metabolites measured in plasma by thin-layer chromatography did not increase with dose, particularly that of the active metabolite isophosphoramide mustard. Furthermore the AUC of the inactive carboxymetabolite did not increase with dose. Interpatient variability of pharmacokinetic parameters was high. Dose-limiting toxicity was myelosuppression at 18 g/m2 total dose with grade 4 neutropenia in five of six patients and grade 4 thrombocytopenia in four of six patients. Therefore the maximum tolerated dose was considered to be 18 g/m2 total dose. There was one CR and eleven PR in twenty-nine evaluable patients (overall response rate 41%). Conclusion: Both the activation and inactivation pathways of ifosfamide are non-linear and saturable at high-doses although the pharmacokinetics of the parent drug itself are dose linear. Ifosfamide doses greater than 14–16 g/m2 per cycle appear to result in a relative decrease of the active metabolite isophosphoramide mustard. These data suggest a dose-dependent saturation or even inhibition of ifosfamide metabolism by increasing high dose ifosfamide and suggest the need for further metabolic studies.

Type of Medium: Electronic Resource

URL: http://dx.doi.org/10.1023/A:1008386000547

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5

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Little to learn from phase II trials in small-cell lung cancer (1999)

Leyvraz, S. ; Stupp, R.

Springer

Annals of oncology 10 (1999), S. 1007-1009

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ISSN: 1569-8041

Source: Springer Online Journal Archives 1860-2000

Topics: Medicine

Type of Medium: Electronic Resource

URL: http://dx.doi.org/10.1023/A:1008306930860

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6

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Phase I multicenter study of combined high-dose ifosfamide and doxorubicin in the treatment of advanced sarcomas (1998)

Leyvraz, S. ; Bacchi, M. ; Cerny, T. ; [et al.]

Springer

Annals of oncology 9 (1998), S. 877-884

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ISSN: 1569-8041

Keywords: gynecological sarcomas ; high-dose doxorubicin ; high-dose ifosfamide ; soft tissue sarcomas

Source: Springer Online Journal Archives 1860-2000

Topics: Medicine

Notes: Abstract Ifosfamide and doxorubicin are the most active agents in the treatment of sarcomas and are characterized by a marked dose-response relationship. The objective of this study was to determine the maximum tolerated dose (MTD) of both agents in combination under granulocyte-macrophage colony-stimulating factor (GM-CSF) cover. Patients and methods: Thirty-three patients with untreated sarcomas (soft tissue: n = 20; gynecological: n = 11; bone: n = 2) were treated with ifosfamide 12 g/m2 by continuous i.v. infusion over five days and doxorubicin with dose escalation from 50 mg/m2 i.v. bolus divided on two days, then to 60 mg/m2 bolus divided on three days. Ifosfamide was reduced to 10 g/m2 and doxorubicin was further escalated up to 90 mg/m2. GM-CSF (5 µg/kg/day subcutaneously) was started 24 hours after chemotherapy and continued for 10 days. Results: The MTD was reached with the combination of ifosfamide at 12 g/m2 and doxorubicin at 60 mg/m2. But with ifosfamide 10 g/m2 and doxorubicin 90 mg/m2 the MTD was not obtained. While severe leukopenia and granulopenia were observed at all-dose levels, severe anemia was more frequently related to the highest dose of ifosfamide. Severe thrombopenia and mucositis were more commonly observed at the highest dose of doxorubicin. Ifosfamide 10 g/m2 and doxorubicin 90 mg/m2 induced WHO grade 4 leukopenia in 58%, grade 3–4 thrombopenia in 42%, and anemia in 31% of cycles. Mucositis was minor in 50% of cycles. The overall response rate among 31 evaluable patients was 55% (95 confidence interval (CI): 36%–73%), with four (13%) complete responders and 13 (42%) partial responders. Response rates based on soft-tissue sarcomas or gynecological sarcomas alone were similar. Ten patients could be treated by elective surgery and/or radiotherapy. The total group of patients reached a median survival of two years, with 25% (SE 8%) survivors after three years. Conclusions: The dose level of ifosfamide 10 g/m2 and doxorubicin 90 mg/m2 with supportive GM-CSF is manageable in a multicenter setting and should be further tested in regular phase II trials, including patients with gynecological and soft-tissue sarcomas. Transient toxicity with myelosuppression should be accepted in order to obtain a high anti-tumor activity of this regimen and a potential improvement in survival.

Type of Medium: Electronic Resource

URL: http://dx.doi.org/10.1023/A:1008464504583

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7

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Sequential administration of temozolomide and fotemustine: Depletion of O6-alkyl guanine-DNA transferase in blood lymphocytes and in tumours (1999)

Gander, M. ; Leyvraz, S. ; Decosterd, L. ; [et al.]

Springer

Annals of oncology 10 (1999), S. 831-838

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ISSN: 1569-8041

Keywords: melanoma ; pharmacodynamics ; pharmacokinetics ; temozolomide

Source: Springer Online Journal Archives 1860-2000

Topics: Medicine

Notes: Abstract Background: The DNA repair protein O6-alkylguanine-DNA alkyl transferase (AT) mediates resistance to chloroethylnitrosoureas. Agents depleting AT such as DTIC and its new analogue temozolomide (TMZ) can reverse resistance to chloroethylnitrosoureas. We report the results of a dose finding study of TMZ in association with fotemustine. Patients and methods: Twenty-four patients with metastatic melanoma or recurrent glioma were treated with escalating dose of oral or intravenous TMZ ranging from 300 to 700 mg/m2, divided over two days. Fotemustine 100 mg/m2 was given intravenously on day 2, 4 hours after TMZ. AT depletion was measured in peripheral blood mononuclear cells (PBMCs) and in selected cases in melanoma metastases and was compared to TMZ pharmacokinetics. Results: The maximum tolerated dose (MTD) of TMZ was 400 mg/m2 (200 mg/m2/d) when associated with fotemustine the 2nd day with myelosuppression as dose limiting toxicity. The decrease of AT level in PBMCs was progressive and reached 34% of pretreatment values on day 2. There was however wide interindividual variability. AT reduction was neither dose nor route dependent and did not appear to be related to TMZ systemic exposure (AUC). In the same patients, AT depletion in tumour did not correlate with the decrease of AT observed in PBMCs. Conclusions: PBMCs may not be used as a surrogate of tumour for AT depletion. Further study should concentrate on the pharmacokinetic pharmacodynamic relationship in tumour to provide the basis for individually tailored therapy.

Type of Medium: Electronic Resource

URL: http://dx.doi.org/10.1023/A:1008304032421

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Ventricular arrhythmia and torsade de pointe: Dose limiting toxicities of the MDR-modulator S9788 in a phase I trial (1998)

Stupp, R. ; Bauer, J. ; Pagani, O. ; [et al.]

Springer

Annals of oncology 9 (1998), S. 1233-1242

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ISSN: 1569-8041

Keywords: arrhythmia ; long QT ; MDR ; P-glycoprotein ; S9788 ; torsade de pointe ; triazineaminopiperidine

Source: Springer Online Journal Archives 1860-2000

Topics: Medicine

Notes: Abstract Background: S9788 is a triazineaminopiperidine derivative capable of reversing multidrug resistance (MDR) in vitro. In preclinical models S9788 was several fold more potent MDR inhibitor than verapamil or cyclosporine. At P-glycoprotein (Pgp) blocking concentrations, S9788 appeared to have only very little toxicity. Patients and methods: In a two step phase I trial we treated 39 patients with refractory cancer with S9788 and bolus doxorubicin. The steps differed mainly in the S9788 infusion duration; in the first part 23 patients received the MDR-reversing drug S9788 over 30 minutes, in the second step of the study 16 patients were administered S9788 over 150 minutes. The doses of S9788 were escalated in cohorts of three patients up to a dose level (DL) of 96 mg/m2 on the 30 minutes infusion, and to 144 mg/m2 on the 150 minutes infusion. The pharmacokinetics of S9788 were determined. Results: With the 30-minute infusion schedule symptomatic cardiac arrhythmia were found to be dose limiting. In all patients at the highest DL transient cardiac repolarization prolongation with a long QT-interval on ECG was demonstrated. With the 150-minute administration schedule, S9788 could be escalated up to 144 mg/m2 without subjective toxicity. However, transient QT prolongation was present in all patients. A third degree AV-block and a QT increase of about 40% occurred at the highest DL. Asymptomatic torsade de pointe (DL 96 mg/m2) was demonstrated on Holter recording in one patient. Theses repolarization disturbances with QT increase were considered dose limiting toxicity and the trial was closed. No arrhythmia related death was noted. Pharmacokinetics were similar with both infusion schedules with a mean alpha half life of 11.3 and 13.2 minutes, for the 30-minute and 150-minute infusion, and a terminal half life of 13.5 and 15 hours, respectively. QTc prolongation duration appeared to be dose-dependent. Conclusions: With the tested infusion schedules, cardiac toxicity, in particular AV-blocks and QT prolongation, leading to ventricular arrhythmia and torsade de pointe, are the dose limiting toxicities of S9788. Our experience together with the observation of asymptomatic torsade de pointe in two other phase I trials of S9788 infused over six hours precluded the further clinical development of S9788.

Type of Medium: Electronic Resource

URL: http://dx.doi.org/10.1023/A:1008495919071

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