Effects of Concomitant Cisplatin and Radiotherapy on Inoperable Non-Small-Cell Lung Cancer.
Schaake-Koning, Caro Ph.D.; van den Bogaert, Walter Ph.D.; Dalesio, Otilia M.Sc.; Festen, Jan Ph.D.; Hoogenhout, Jaap Ph.D.; van Houtte, Paul M.D.; Kirkpatrick, Anne M.S.; Koolen, Mia M.D.; Maat, Ben Ph.D.; Nijs, Arie M.D.; Renaud, Alain M.D.; Rodrigus, Patrick M.D.; Schuster-Uitterhoeve, Lon M.D.; Sculier, Jean-Paul M.D.; van Zandwijk, Nico Ph.D.; Bartelink, Harry Ph.D.
[Article]
New England Journal of Medicine.
326(8):524-530, February 20, 1992.
(Format: HTML, PDF)
Background and Methods. Cisplatin (cis-diamminedichloroplatinum) has been reported to enhance the cell-killing effect of radiation, an effect whose intensity varies with the schedule of administration. We randomly assigned 331 patients with nonmetastatic inoperable non-small-cell lung cancer to one of three treatments: radiotherapy for two weeks (3 Gy given 10 times, in five fractions a week), followed by a three-week rest period and then radiotherapy for two more weeks (2.5 Gy given 10 times, five fractions a week); radiotherapy on the same schedule, combined with 30 mg of cisplatin per square meter of body-surface area, given on the first day of each treatment week; or radiotherapy on the same schedule, combined with 6 mg of cisplatin per square meter, given daily before radiotherapy.
Results. Survival was significantly improved in the radiotherapy-daily-cisplatin group as compared with the radiotherapy group (P = 0.009): survival in the radiotherapy-daily-cisplatin group was 54 percent at one year, 26 percent at two years, and 16 percent at three years, as compared with 46 percent, 13 percent, and 2 percent, respectively, in the radiotherapy group. Survival in the radiotherapy-weekly-cisplatin group was intermediate (44 percent, 19 percent, and 13 percent) and not significantly different from survival in either of the other two groups. The survival benefit of daily combined treatment was due to improved control of local disease (P = 0.003). Survival without local recurrence was 59 percent at one year and 31 percent at two years in the radiotherapy-daily-cisplatin group; 42 percent and 30 percent, respectively, in the radiotherapy-weekly-cisplatin group; and 41 percent and 19 percent, respectively, in the radiotherapy group. Cisplatin induced nausea and vomiting in 86 percent of the patients given it weekly and in 78 percent of those given it daily; these effects were severe in 26 percent and 28 percent, respectively.
Conclusions. Cisplatin, given daily in combination with the radiotherapy described here to patients with nonmetastatic but inoperable non-small-cell lung cancer, improved rates of survival and control of local disease at the price of substantial side effects. (N Engl J Med 1992;326: 524-30.)
NON-SMALL-CELL lung cancer is the most frequent cause of death due to cancer in men in the Western world, and its incidence among women is rapidly increasing. The poor prognosis of patients with locally advanced tumors has remained essentially unchanged in recent decades. At diagnosis, only 25 percent of all patients are considered candidates for surgery.1 The five-year survival rate is 25 percent among patients with resectable disease.2 Radiotherapy is frequently considered for patients with localized inoperable disease; they are selected on the basis of prognostic factors, such as cancer stage (TNM status), performance status, weight loss, and other factors. [horizontal ellipsis]
Owned, published, and (C) copyrighted, 1992, by the MASSACHUSETTS MEDICAL SOCIETY
