Phase II study of doxifluridine in advanced colorectal adenocarcinoma.

Abele, Reto; Alberto, P.; Kaplan, Susanna; Siegenthaler, Paul‐André; Hofmann, V.; Ryssel, H J; Hartmann, D; Holdener, Eduard E.; Cavalli, F.

doi:10.1200/jco.1983.1.12.750

Cited by 43 publications

(13 citation statements)

References 5 publications

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“…Our results are similar to the reported trials in the treatment of advanced colorectal carcinoma [8,9,13,15]. There is no advantage for response dependent on routes of administra tion, but the one hour infusion showed low toxicities in contrast to the bolus injection and 6-hours infusion.…”

Section: Discussionsupporting

confidence: 80%

“…In several contributions [8,9,13,15] as well as in our own previous experiences [14] it was clearly outlined that 5'dFUR is active for treatment of colorectal carcinoma. However, the optimal dose and route of application is still controversial.…”

Section: Discussionmentioning

confidence: 99%

“…Cytotoxic activity varies considerably, the highest occurring in tumor tissue and small intestine [5], In a phase-I clinical trial using a daily schedule with rapid intravenous injections for five consecutive days, doses were escalated up to 5 g/m2. Granulocytopenia as well as stomatites were found to be dose limiting, and other toxic effects con sisted of nausea/vomiting, central nervous system symptoms and ECG changes [6], Disease-oriented phase-II trials have demonstrated cytotoxic activity of 5'dFUR in a variety of solid tumors including ovarian carcinoma [7], colorectal carcinoma [8,9], malignant melanoma [10], head and neck [11] as well as breast carcinoma [12] if the drug was administered at a daily x 5 schedule for one hour infusion or for bolus injection. The dose limiting toxicities encountered in these trials were leukopenia, stomati tis and cerebellar ataxia.…”

mentioning

confidence: 99%

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Prospective Multicenter Phase-Ill Trial of Doxifluridine (5’dFUR) versus 5-Fluorouracil in Patients with Advanced Colorectal Carcinoma

Schuster¹,

Heim²,

Dombernowski

et al. 1991

Oncol Res Treat

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Doxifluridine (5’dFUR) is a new fluropyrimidine derivative with significant antitumor activity in animal models. Preliminary studies with bolus injections, one, six hours and continous infusion, have indicated that doxifluridine is active in a variety of refractory tumors. In a randomized multicentre trial 71 previously untreated patients with advanced colorectal carcinoma were allocated to receive doxifluridine (5’dFUR) 4,000 mg/m² or 5-fluorouracil (5-FU) 450 mg/m² as one hour intravenous infusion daily for 5 consecutive days every 4 weeks. In 61 evaluable patients (5’dFUR 31 and 5-FU 30) non-complete remission was treated with 5’dFUR and 2/30 (7%) of patients treated with 5-FU. The median survival of the 5’dFUR arm (all patients) was not statistically different compared to 5-FU (52.5 and 42.5 weeks). Gastrointestinal adverse events were common in both treatment groups. Hematotoxicity occurred in both schedules with a higher incidence for the 5’dFUR arm. Additionally, low grade toxicity (WHO grade 1–2) of skin, neurotoxic symptoms and cardiotoxicity occurred in the 5’dFUR arm only. 5’dFUR in dosage and schedule used in this study is an active agent for advanced colorectal carcinoma but efficacy is accompanied by more pronounced adverse reactions.

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Section: Discussionsupporting

confidence: 80%

Section: Discussionmentioning

confidence: 99%

mentioning

confidence: 99%

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Prospective Multicenter Phase-Ill Trial of Doxifluridine (5’dFUR) versus 5-Fluorouracil in Patients with Advanced Colorectal Carcinoma

Schuster¹,

Heim²,

Dombernowski

et al. 1991

Oncol Res Treat

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“…The cardiotoxic effects of 5-FU have been extensively reported [3,4,5,6,7,8,9]. More recently, cardiotoxicity has been reported with doxifluridine [10], tegafur [11] and the oral fluoropyrimidines capecitabine [12,13,14,15,16] and UFT [17,18,19], predominantly in patients with colorectal cancer. We report a case of cardiotoxicity during the first cycle of capecitabine treatment in a woman with metastatic breast cancer, followed by a review of the available literature and a discussion of the possible pathophysiology of this cardiotoxicity and its implications for practice.…”

Section: Introductionmentioning

confidence: 99%

Cardiac Toxicity with Capecitabine, Vinorelbine and Trastuzumab Therapy: Case Report and Review of Fluoropyrimidine-Related Cardiotoxicity

Brun-Ly

Martin²,

Venat-Bouvet³

et al. 2009

Oncology

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A 45-year-old woman presented with a metastatic breast carcinoma and was treated with capecitabine, oral vinorelbine and trastuzumab combination therapy. The initial echocardiogram and the ECG were considered normal. She began treatment with 3-weekly cycles of the combination therapy. After the fourth dose of capecitabine, she presented with severe chest and arm pain, which was responsive to nitroglycerine spray. ECG at admission demonstrated tachycardia with ST-segment elevation suggesting ischemia. The clinical symptoms returned to baseline after a few hours and within 24 h the ECG showed inverted T in leads V3–V6. Cardiac ultrasonography revealed hypokinesia in the left ventricle without segmentary hypokinesia, with mildly reduced global systolic function, which normalized 1 week later. Two weeks later, she was rechallenged with capecitabine. After the fourth dose, the patient developed chest pain. ECG showed infero-apico-lateral injury, which normalized after administration of nitrates, nicorandil and verapamil and discontinuation of capecitabine. This case suggests that capecitabine can lead to the cardiotoxicity characteristic of other fluoropyrimidines. Therefore, it is important to inform patients about the risk of angina-like chest pain, to stop treatment immediately if symptoms occur, and to monitor the patient in hospital. Fluoropyrimidine rechallenge should be avoided because of the risk of ischemic event or sudden death.

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“…x 5 days in good-or poor-risk patients, respectively, demonstrated that 5dFUR has def inite activity in a variety of tumors usually sensitive to fluoropyrimidines, such as carcinoma of the breast [20], colon-rectum [21 ], and of the head and neck district [22], Furthermore, some comparative trials with 5FU for 5 consecutive days were carried out in colorectal cancer [23,24], Also in these trials, the infusion time seemed to affect both type and severity of toxicity. Indeed, a higher occur rence of neurologic (48%) and cardiac toxicity (19%) as compared to the parent compound was reported when 5dFUR was administered as intravenous bolus [23], while these side effects affected 23 and 1% of patients, respec tively, when 5dFUR was given as 1-hour intravenous infusion [24], In advanced SCCHN, the combination of CDDP and continuous intravenous infusion 5FU, with or without the addition of L-FA, has demonstrated to be a very active treatment itself, for unresectable or recurrent disease [4][5][6][7][8].…”

mentioning

confidence: 99%

Dose–Finding Study of 5’-Deoxy-5-Fluorouridine in Combination with Fixed Doses of Cisplatin and <i>L</i>-Folinic Acid for the Treatment of Advanced or Recurrent Squamous Cell Carcinoma of the Head and Neck

Comella

Biglietto

Scarpati³

et al. 1995

Oncology

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In order to assess the maximum tolerated dose of 5’-deoxy-5-fmorouridine (5dFUR) combined with a cisplatin (20 mg/m² i.v.) and L-folinic acid (100 mg/m² i.v.), 5-day schedule 19 consecutive chemotherapy-naive patients affected by advanced or recurrent carcinoma of the head and neck were entered in this phase I trial. Doses of 5dFUR were escalated from a starting level of 2,000 mg/m²/day up to 3,000 and 5,000 mg/m²/day. At the latter step the dose-limiting acute toxicities were stomatitis and diarrhea, which were of WHO grade 3–4 and occurred in 3 and 1 out of 4 evaluated patients, respectively. Other grade 3 acute toxicities were leukopenia, anemia, renal impairment, and neurologic symptoms, observed in 1 patient each. Furthermore, one possibly treatment-related death was registered among patients entered in the highest dose level. Eleven out of 19 patients (58%; 95% CI: 34–80%) showed a complete (2 cases) or partial (9 cases) response to this treatment, regardless of the 5dFUR dosage employed. From our results we may define the maximum tolerated dose of 5dFUR to be associated with cisplatin and L-folin acid used in this trial as 3,000 mg/m²/day x 5 days. Assessment of the real activity of this combination chemotherapy deserves further studies.

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Phase II study of doxifluridine in advanced colorectal adenocarcinoma.

Cited by 43 publications

References 5 publications

Prospective Multicenter Phase-Ill Trial of Doxifluridine (5’dFUR) versus 5-Fluorouracil in Patients with Advanced Colorectal Carcinoma

Prospective Multicenter Phase-Ill Trial of Doxifluridine (5’dFUR) versus 5-Fluorouracil in Patients with Advanced Colorectal Carcinoma

Cardiac Toxicity with Capecitabine, Vinorelbine and Trastuzumab Therapy: Case Report and Review of Fluoropyrimidine-Related Cardiotoxicity

Dose–Finding Study of 5’-Deoxy-5-Fluorouridine in Combination with Fixed Doses of Cisplatin and <i>L</i>-Folinic Acid for the Treatment of Advanced or Recurrent Squamous Cell Carcinoma of the Head and Neck

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Phase II study of doxifluridine in advanced colorectal adenocarcinoma.

Cited by 43 publications

References 5 publications

Prospective Multicenter Phase-Ill Trial of Doxifluridine (5’dFUR) versus 5-Fluorouracil in Patients with Advanced Colorectal Carcinoma

Prospective Multicenter Phase-Ill Trial of Doxifluridine (5’dFUR) versus 5-Fluorouracil in Patients with Advanced Colorectal Carcinoma

Cardiac Toxicity with Capecitabine, Vinorelbine and Trastuzumab Therapy: Case Report and Review of Fluoropyrimidine-Related Cardiotoxicity

Dose–Finding Study of 5&#8217;-Deoxy-5-Fluorouridine in Combination with Fixed Doses of Cisplatin and <i>L</i>-Folinic Acid for the Treatment of Advanced or Recurrent Squamous Cell Carcinoma of the Head and Neck

Contact Info

Product

Resources

About

Dose–Finding Study of 5’-Deoxy-5-Fluorouridine in Combination with Fixed Doses of Cisplatin and <i>L</i>-Folinic Acid for the Treatment of Advanced or Recurrent Squamous Cell Carcinoma of the Head and Neck