首页> 外文期刊>Pharmacology and Toxicology: An International Journal >The drinking water chlorination by-products 3,4-dichloro-5-hydroxy-2(5H)-furanone(mucochloric acid) and 3-chloro-4-(dichloromethyl)-5-hydroxy-2(5H)-furanone do not induce preneoplastic or neoplastic intestinal lesions in F344 rats, balb/ca mice or C5
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The drinking water chlorination by-products 3,4-dichloro-5-hydroxy-2(5H)-furanone(mucochloric acid) and 3-chloro-4-(dichloromethyl)-5-hydroxy-2(5H)-furanone do not induce preneoplastic or neoplastic intestinal lesions in F344 rats, balb/ca mice or C5

机译:饮用水氯化副产物3,4-二氯-5-羟基-2(5H)-呋喃酮(粘氯酸)和3-氯-4-(二氯甲基)-5-羟基-2(5H)-呋喃酮没有诱导F344大鼠,balb / ca小鼠或C5的肿瘤前或肿瘤性肠病变

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Epidemiological studies indicate an association between exposure to chlorinated drinking water and risk of intestinal cancer. In order to study this experimentally, we have examined the effects of 3,4-dichloro-5-hydroxy-2[5H]-furanone (mucochloric acid, MCA) and 3-chloro-4-(dichloromethyl)-5-hydroxy-2[5H]-furanone (MX), mutagenic and genotoxic compounds in drinking water, on aberrant crypt foci and tumours in the intestines of male F344 rats and Balb/cA mice, and C57BL/6J-Min (multiple intestinal neoplasia)/+ mice of both sexes, in six independent experiments. In some experiments the effects of MCA and MX on aberrant crypt foci induced by the colon carcinogens 1,2-dimethylhydrazine or its metabolite azoxymethane were also studied. Neither MCA nor MX alone induced aberrant crypt foci or intestinal tumours when given in drinking water. With this route of exposure neither MCA nor MX, when given in combination with 1,2-dimethylhydrazine or azoxymethane, had any effect on the induction or growth of the aberrant crypt foci. Drinking water exposure of MX did not affect the number or growth of aberrant crypt foci or intestinal tumours in the Minl+ mice. When administered intrarectally MCA had a weak inducing effect on aberrant crypt foci in the colons of Balb/cA mice. Exposure to MCA and MX intrarectally apparently promoted the growth of aberrant crypt foci both in rats and mice, increasing the crypt multiplicity, aberrant crypts/aberrant crypt foci. Based on an overall evaluation of these experiments, the intestinal tract, at least in rats and mice, seems not to be a main target organ for effects of MCA or MX on preneoplastic or neoplastic development.
机译:流行病学研究表明,接触氯化饮用水与肠道癌风险之间存在关联。为了进行实验研究,我们研究了3,4-dichloro-5-hydroxy-2 [5H]-呋喃酮(粘氯酸,MCA)和3-chloro-4-(dichloromethyl)-5-hydroxy- 2 [5H]-呋喃酮(MX),饮用水中的致突变性和遗传毒性化合物,对雄性F344大鼠和Balb / cA小鼠以及C57BL / 6J-Min(多发性肠肿瘤)的肠道隐窝灶和肿瘤有影响在六个独立的实验中,发现了两个性别的老鼠。在某些实验中,还研究了MCA和MX对结肠癌致癌剂1,2-二甲基肼或其代谢产物甲氧基甲烷诱导的异常隐窝灶的影响。饮用水中,单独使用MCA和MX均不会诱发隐窝病灶或肠道肿瘤。通过这种暴露途径,当MCA和MX与1,2-二甲基肼或叠氮甲烷联合使用时,对异常隐窝灶的诱导或生长均没有任何影响。饮用水暴露于MX不会影响Minl +小鼠中异常隐窝灶或肠道肿瘤的数量或生长。当直肠内给药时,MCA对Balb / cA小鼠结肠中隐窝灶的诱导作用较弱。直肠内暴露于MCA和MX显然促进了大鼠和小鼠异常隐窝灶的生长,从而增加了隐窝多样性,异常隐窝/异常隐窝灶。根据对这些实验的总体评估,至少在大鼠和小鼠中,肠道似乎不是MCA或MX对肿瘤前或肿瘤发展的主要靶器官。

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