[Histopathological studies on antitumor effect of tegafur administered by continuous intravenous infusion].

Nihon Gan Chiryo Gakkai shi Pub Date : 1990-06-20
A Yagawa
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Abstract

The effects of preoperative treatment by continuous intravenous infusion of Tegafur, the antagonist of DNA synthesis, were histopathologically studied in 34 patients with gastric cancer. Histologically the treatment was found to be effective in 41.2% of patients with cancer invasion in the mucosa, 58.8% in the submucosa, 61.3% in the muscularis propria, 59.3% in the subserosa and 86.9% of those with metastatic lymph nodes. The treatment was effective, when assessed in terms of the histological type of cancer, in 90.9% of cancers of the differentiated type (papillary adenocarcinoma, well differentiated tubular adenocarcinoma and moderately differentiated tubular adenocarcinoma) and 47.8% of those of the poorly differentiated type (poorly differentiated adenocarcinoma, mucinous adenocarcinoma and signet-ring cell carcinoma), showing a higher rate of efficacy in the differentiated type cancers. Meanwhile, even among patients with cancer of poorly differentiated type, a high efficacy rate (90.0%) was found in those with metastatic cancer of the lymph nodes. No relationship was found between the total doses of Tegafur and histological effects. There was a tendency, however, for a higher frequency of a good response in patients administered more than 4,000 mg of Tegafur. In the patients with a histologically positive effect, 5-FU concentration in the tumor tissue was higher than 0.071 microgram/g. However, some patients showed no response despite a high concentration. This finding suggested that sensitivity to 5-FU and 5-FU metabolism vary depending on the tumor. The inhibitory effect of Tegafur on DNA synthesis is produced through inhibition of thymidylate synthase (TS) by the Tegafur metabolite FdUMP.(ABSTRACT TRUNCATED AT 250 WORDS)

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连续静脉输注替加福抗肿瘤作用的组织病理学研究。
对34例胃癌患者术前持续静脉输注DNA合成拮抗剂替加富的治疗效果进行了组织病理学观察。组织学上,41.2%的肿瘤浸润于粘膜,58.8%浸润于粘膜下层,61.3%浸润于固有肌层,59.3%浸润于浆膜下,86.9%浸润于淋巴结转移。从肿瘤的组织学类型来看,90.9%的分化型(乳头状腺癌、高分化管状腺癌和中分化管状腺癌)和47.8%的低分化型(低分化腺癌、粘液腺癌和印戒细胞癌)治疗有效,分化型肿瘤的有效率更高。同时,即使在低分化型癌症患者中,淋巴结转移癌的有效率也很高(90.0%)。没有发现替加富总剂量与组织学效应之间的关系。然而,有一种趋势是,服用超过4000毫克替加富的患者出现良好反应的频率更高。组织学阳性患者肿瘤组织中5-FU浓度高于0.071微克/克。然而,尽管浓度很高,但有些患者没有反应。这一发现表明,对5-FU的敏感性和5-FU的代谢因肿瘤而异。替加氟对DNA合成的抑制作用是通过替加氟代谢物FdUMP抑制胸苷酸合成酶(TS)产生的。(摘要删节250字)
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