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. 1999 Nov;26(13):2009-14.

[Second primary malignancy after surgical adjuvant therapy for gastric cancer]

[Article in Japanese]
Affiliations
  • PMID: 10584564

[Second primary malignancy after surgical adjuvant therapy for gastric cancer]

[Article in Japanese]
J Fujimoto. Gan To Kagaku Ryoho. 1999 Nov.

Abstract

Immunopotentiators are expected to intensify the effects of chemotherapy, but anticancer agents are in greater or lesser degree carcinogenic in humans. The carcinogenic risk after adjuvant chemo-immunotherapy was examined in 786 gastric cancer patients who underwent curative gastrectomy between 1963 and 1981. They consisted of 420 patients without any chemo- or immunotherapy (cont group), 302 with chemotherapy (chem group) with mitomycin C and/or fluorinated pyrimidines, and 64 with chemo-immunotherapy (chem-immu group) with both chemotherapy and immuno-potentiator (s), levamisole or PSK and/or OK-432. The incidence of cancers other than gastric cancer 5 or more years after gastrectomy was 9 out of 64 in the chem-immu group (14.1%), which was higher than the 25 out of 302 in the chem group (8.3%) and significantly higher than the 27 out of 420 in the cont group (6.4%) (p < 0.05). The 5/10-year survival rate after gastrectomy was 76.0%/72.5% in the chem-immu group, which was significantly higher than the 66.1% /59.4% in the chem group and the 64.7%/59.3% in the cont group (p < 0.05). Among 215 patients under 50 years of age, the survival rate was 72.7%/65.6% in the chem group, which was significantly lower than the 75.0%/71.7% in the cont group (p < 0.01) and lower than the 81.9%/81.9% in the chem-immu group. However, the incidence of a second malignancy showed a tendency to increase in the order of the cont, chem and chem-immu groups.

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