AN EVALUATION OF THE EFFECTIVENESS AND SAFETY OF RAZOXANE WHEN USED AS AN ADJUNCT TO SURGERY IN COLORECTAL-CANCER - REPORT OF A CONTROLLED RANDOMIZED STUDY OF 603 PATIENTS

被引：5

作者：

KINGSTON, RD

FIELDING, JWL

PALMER, MK

机构：

[1] Department of Clinical Studies, Trafford General Hospital, Manchester

[2] Surgical Immunology Unit, Queen Elizabeth Hospital, Birmingham

[3] ICI Pharmaceuticals, Macclesfield, Alderley Park

来源：

INTERNATIONAL JOURNAL OF COLORECTAL DISEASE | 1993年 / 8卷 / 02期

关键词：

D O I：

10.1007/BF00299338

中图分类号：

R57 [消化系及腹部疾病];

学科分类号：

摘要：

A prospective controlled randomised trial to evaluate the effectiveness and safety of razoxane is reported. Some 603 patients with colo-rectal cancer having curative surgery entered the study, and all have been followed up for a minimum of five years. Statistical analysis showed that razoxane treatment had no effect either beneficial or adverse on the rates of recurrence or on five year survival of patients with colo-rectal cancer. It is possible that a more prolonged course of razoxane might have significantly influenced survival. The incidence of severe adverse reaction was low but it is of concern that one patient developed leukaemia. Should razoxane be considered for future use it is recommended that continuous low dose therapy be given for no longer than 12 months. No renal, hepatic, pulmonary or cardiac toxicity was noted.

引用

页码：106 / 110

页数：5

共 19 条

[1]

Moertel C.G., Fleming T.R., Mac Donald J.S., Heller D.G., Laurie J.A., Goodman P.J., Ungerleider J.S., Emerson W.A., Tormey D.C., Glick J.H., Veeder M.H., Mailliard J.A., Levamisole and fluorouracil for adjuvant therapy of resected colon cancer, N Engl J Med, 322, pp. 352-358, (1990)

[2]

Whitehouse J.M.A., Risk of leukaemia associated with cancer chemotherapy, BMJ, 290, pp. 261-263, (1985)

[3]

Geary C.G., Lymphoma and leukaemia due to drugs, Br J Hosp Med, 24, pp. 538-547, (1980)

[4]

Bakowski M.T., I.C.R.F. 159 (+1,2-di (3,5-dioxopiperazin-l-yl)-propane. N.S.C.-129943

[5]

Razoxane, Cancer Treat Rep, 3, pp. 95-107, (1976)

[6]

Gilbert J.M., Hellmann K., Evans M., Cassell P.G., Stoodley B., Ellis H., Wastell C., Adjuvant oral razoxane (I.C.R.F. 159) in resectable colorectal cancer, Cancer Chemother Pharmacol, 8, pp. 293-299, (1982)

[7]

Gilbert J.M., Hellmann K., Evans M., Cassell P.G., Taylor R.H., Stoodley B., Ellis H., Wastell C., Randomised trial of oral adjuvant razoxane (I.C.R.F. 159) in resectable colo-rectal cancer: Five year follow-up, Br J Surg, 73, pp. 446-450, (1986)

[8]

Hellmann K., Burrage K., Control of malignant metastases by I.C.R.F. 159, Nature, 224, pp. 273-275, (1969)

[9]

Salsbury A.J., Burrage K., Hellmann K., Inhibition of metastatic spread by I.C.R.F. 159: Selective deletion of a malignant characteristic, BMJ, 34, pp. 344-346, (1970)

[10]

LeServe A.W., Hellmann K., Metastases and the normalisation of tumour blood vessels by I.C.R.F. 159 a new type of drug action, BMJ, 1, pp. 597-601, (1972)

← 1 2 →