Takechi T, Nakano K, Uchida J, Mita A, Toko K, Takeda S, Unemi N, Shirasaka T
Anticancer and Antimicrobials Research Laboratory, Taiho Pharmaceutical Co. Ltd., Tokushima, Japan.
Cancer Chemother Pharmacol. 1997;39(3):205-11. doi: 10.1007/s002800050561.
S-1, a new oral antitumor agent, is composed of 1-(2-tetrahydrofuryl)-5-fluorouracil (Tegafur, FT), 5-chloro-2,4-dihydroxypyridine (CDHP) and potassium oxonate (Oxo) in a molar ratio of 1:0.4:1. FT which is a masked compound of 5-fluorouracil (5-FU) acts as an effector, while both CDHP and Oxo which do not have antitumor activity themselves act as modulators. In this study, the antitumor activity and intestinal toxicity of S-1 were investigated using experimental tumor models in rats, and compared with those of other oral fluoropyrimidines, namely 5-FU, FT, FCD (1 M FT/0.4 M CDHP) and UFT (combination of FT and uracil). In rats bearing subcutaneous Yoshida sarcoma, S-1 inhibited tumor growth at the lowest dose (ED50 value: S-1 5, UFT 22, FT 82, FCD 5, and 5-FU 19 mg/kg per day), and induced the least host body weight suppression, leading to the highest therapeutic index (TI) (S-1 4.5, UFT 1.4, FT 1.8, FCD 2.0, and 5-FU 1.4). S-1 also showed a higher therapeutic effect than UFT against AH-130 and Sato lung carcinoma. After administration of S-1 and UFT at equitoxic doses, S-1 showed a higher and more prolonged concentration of 5-FU than UFT both in plasma (AUC0-infinity: S-1 28 nmolh/ml, UFT 15 nmol.h/ml) and in tumor tissue (AUC0-infinity: S-1 95 nmolh/g tissue, UFT 52 nmolh/g tissue), leading to a higher 5-FU level incorporated into the RNA fraction (F-RNA level) in tumor tissue (AUC0-24: S-1 7.0 nmolh/mg RNA, UFT 4.3 nmolh/mg RNA) and 5-8% higher thymidylate synthase (TS) inhibition in tumor tissue at every time-point through 24 h. Compared with other oral fluoropyrimidines after administration of the maximal tolerable dose (MTD), S-1 caused the lowest rates of intestinal toxicities, such as diarrhea and occult blood in feces. S-1 also showed a higher antitumor effect on Yoshida sarcoma implanted intracolonically than UFT at an equitoxic dose (tumor weight: S-1 64 +/- 30 mg, UFT 133 +/- 52 mg; P < 0.05). These results suggest that CDHP, which is a potent inhibitor of 5-FU degradation, increases the antitumor activity of FT, and that Oxo, which is an inhibitor of 5-FU phosphorylation, locally protects the gastrointestinal tract from 5-FU-induced toxicity without decreasing the antitumor activity.
S-1是一种新型口服抗肿瘤药物,由1-(2-四氢呋喃基)-5-氟尿嘧啶(替加氟,FT)、5-氯-2,4-二羟基吡啶(CDHP)和奥索酸钾(Oxo)按1:0.4:1的摩尔比组成。FT是5-氟尿嘧啶(5-FU)的一种掩蔽化合物,起效应剂作用,而本身无抗肿瘤活性的CDHP和Oxo均起调节剂作用。在本研究中,使用大鼠实验性肿瘤模型研究了S-1的抗肿瘤活性和肠道毒性,并与其他口服氟嘧啶类药物,即5-FU、FT、FCD(1 M FT/0.4 M CDHP)和优福定(FT与尿嘧啶的组合)进行了比较。在携带皮下吉田肉瘤的大鼠中,S-1以最低剂量抑制肿瘤生长(半数有效剂量值:S-1为5、优福定为22、FT为82、FCD为5、5-FU为19 mg/kg/天),并且引起的宿主体重抑制最小,从而导致最高的治疗指数(TI)(S-1为4.5、优福定为1.4、FT为1.8、FCD为2.0、5-FU为
