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通过对小鼠进行皮肤涂抹以及对大鼠进行灌胃,研究羟基化烷基亚硝基脲和亚硝基恶唑烷酮的致癌性。

Carcinogenicity of hydroxylated alkylnitrosoureas and of nitrosooxazolidones by mouse skin painting and by gavage in rats.

作者信息

Lijinsky W, Reuber M D

出版信息

Cancer Res. 1983 Jan;43(1):214-21.

PMID:6847770
Abstract

The carcinogenic effectiveness of a number of nitrosoalkylamides related to nitrosoethylurea and nitroso-n-propylurea has been compared by topical application to Swiss mice and by intragastric administration to F344 rats. Nitrosohydroxyethylurea and the related cyclic nitrosamide, nitrosooxazolidone, were as potent as nitrosoethylurea as skin carcinogens, although the latter was a much weaker mutagen to Salmonella. When administered p.o., nitrosooxazolidone induced mainly forestomach tumors in rats, while nitrosohydroxyethylurea was very broadly acting, inducing neoplasms of the lung, forestomach, glandular stomach, colon, duodenum, and bone (osteogenic sarcomas). Nitroso-2-hydroxypropylurea, nitroso-3-hydroxypropylurea, and nitroso-5-methyloxazolidone were all much more potent carcinogens on mouse skin than was nitroso-n-propylurea, nitroso-5-methyloxazolidone being somewhat less effective than the nitrosoureas; the mutagenicity to Salmonella seemed not to be quantitatively related to carcinogenicity. Nitroso-5-methyloxazolidone given p.o. to rats induced mainly forestomach neoplasms and a few neoplasms of the duodenum, whereas similar treatment of rats with nitroso-2-hydroxypropylurea induced a high incidence of neoplasms of the thymus, some of the forestomach, and few at any other site.

摘要

通过对瑞士小鼠进行局部涂抹以及对F344大鼠进行胃内给药,比较了多种与亚硝基乙基脲和亚硝基正丙基脲相关的亚硝基烷基酰胺的致癌效力。亚硝基羟乙基脲和相关的环状亚硝酰胺——亚硝基恶唑烷,作为皮肤致癌物,其效力与亚硝基乙基脲相当,尽管后者对沙门氏菌的致突变性要弱得多。经口服给药时,亚硝基恶唑烷主要诱导大鼠前胃肿瘤,而亚硝基羟乙基脲的作用范围非常广泛,可诱导肺、前胃、腺胃、结肠、十二指肠和骨骼(骨肉瘤)的肿瘤。亚硝基-2-羟丙基脲、亚硝基-3-羟丙基脲和亚硝基-5-甲基恶唑烷对小鼠皮肤的致癌性均比亚硝基正丙基脲强得多,亚硝基-5-甲基恶唑烷的效力略低于亚硝脲类;对沙门氏菌的致突变性似乎与致癌性没有定量关系。给大鼠口服亚硝基-5-甲基恶唑烷主要诱导前胃肿瘤和少数十二指肠肿瘤,而用亚硝基-2-羟丙基脲对大鼠进行类似处理则诱导胸腺肿瘤的高发病率,还有一些前胃肿瘤,在其他任何部位的肿瘤都很少。

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