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阿司匹林对雄性F344大鼠膀胱致癌作用中N-[4-(5-硝基-2-呋喃基)-2-噻唑基]甲酰胺引发及糖精钠促癌的抑制作用。

Inhibition by aspirin of N-[4-(5-nitro-2-furyl)-2-thiazolyl]formamide initiation and sodium saccharin promotion of urinary bladder carcinogenesis in male F344 rats.

作者信息

Sakata T, Hasegawa R, Johansson S L, Zenser T V, Cohen S M

出版信息

Cancer Res. 1986 Aug;46(8):3903-6.

PMID:3731063
Abstract

N-[4-(5-Nitro-2-furyl)-2-thiazolyl]formamide (FANFT) is metabolically activated by several enzyme systems, including prostaglandin H synthase. Aspirin is an inhibitor of prostaglandin H synthase and has been shown to inhibit FANFT-induced bladder carcinogenesis when coadministered in the diet. To further evaluate the effects of aspirin on bladder carcinogenesis in the rat, we have coadministered aspirin with FANFT during the initiation phase and with sodium saccharin during the promotion phase of carcinogenesis. FANFT was administered in the diet at a level of 0.2% for 6 weeks as the initiator and sodium saccharin was administered in the diet at a level of 5% for 61 weeks as promoting stimulus. Aspirin was administered at a level of 0.5% with FANFT or with sodium saccharin, and appropriate control groups were included. Weanling male Fischer 344 rats were utilized and the chemicals were added to Agway Prolab 3000 rat chow. A 1-week interval was included between the FANFT and sodium saccharin administration during which the rats received either aspirin containing diet or control chow, depending on the treatment regimen of the group. Thirty rats were included in each group at the beginning of the experiment, except for the control group which contained 40. Rats given FANFT followed by saccharin had a bladder carcinoma incidence of 83%. Rats given aspirin with FANFT but not with saccharin had a carcinoma incidence of 20% and the rats fed aspirin with the saccharin but not with the FANFT had an incidence of 28%. FANFT followed by control diet resulted in a bladder carcinoma incidence of 10%, as was true for the rats given FANFT plus aspirin followed by control diet. However, the hyperplastic effects induced in the bladder epithelium by saccharin without prior FANFT administration were inhibited by coadministration with aspirin. These results indicate that aspirin inhibits both FANFT initiation and sodium saccharin promotion of bladder carcinogenesis, but the mechanisms involved would most probably be different for each.

摘要

N-[4-(5-硝基-2-呋喃基)-2-噻唑基]甲酰胺(FANFT)可被包括前列腺素H合酶在内的多种酶系统代谢激活。阿司匹林是前列腺素H合酶的抑制剂,当与FANFT同时添加到饮食中时,已显示出可抑制FANFT诱导的膀胱癌发生。为了进一步评估阿司匹林对大鼠膀胱癌发生的影响,我们在致癌作用的起始阶段将阿司匹林与FANFT同时给药,并在促进阶段将其与糖精钠同时给药。FANFT作为引发剂以0.2%的水平添加到饮食中持续6周,糖精钠作为促癌刺激物以5%的水平添加到饮食中持续61周。阿司匹林以0.5%的水平与FANFT或糖精钠同时给药,并设置了适当的对照组。使用断乳雄性Fischer 344大鼠,将化学物质添加到Agway Prolab 3000大鼠饲料中。在FANFT和糖精钠给药之间有1周的间隔期,在此期间,大鼠根据组的治疗方案接受含阿司匹林的饮食或对照饲料。实验开始时每组有30只大鼠,对照组有40只。先给予FANFT再给予糖精的大鼠膀胱癌发生率为83%。给予阿司匹林与FANFT但不与糖精的大鼠癌发生率为20%,给予阿司匹林与糖精但不与FANFT的大鼠发生率为28%。FANFT后给予对照饮食的大鼠膀胱癌发生率为10%,给予FANFT加阿司匹林后再给予对照饮食的大鼠也是如此。然而,在没有预先给予FANFT的情况下,糖精诱导的膀胱上皮增生效应可被与阿司匹林同时给药所抑制。这些结果表明,阿司匹林可抑制FANFT引发的以及糖精钠促进的膀胱癌发生,但其中涉及的机制很可能对每种情况都有所不同。

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