1975
DOI: 10.1093/jnci/55.3.705
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Tumorigenesis by Oxygenated Nitrosopiperidines in Rats2

Abstract: Three oxygenated N-nitrosopiperidines--nitroso-3-piperidinol, nitroso-4-piperidinol, and nitroso-4-piperidone--were prepared and given in drinking water at equivalent molar doses to Sprague-Dawley rats. All were potent carcinogens, 100% of the rats developed tumors in all treatment groups. Nitroso-3-piperidinol resembled nitrosopiperidine in inducing a high incidence of tumors of the nasal cavity and upper alimentary tract, and a few liver tumors. Nitroso-4-piperidinol and nitroso-4-piperidone caused a high in… Show more

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Cited by 19 publications
(12 citation statements)
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“…The carcinogenicity of 3-hydroxy- N -nitrosopiperidine was evaluated in rats (15 males, 14 females) after administration via drinking water for 36 weeks (total study duration 50 weeks) resulting in adjusted daily doses of 2.38 (males) and 3.40 mg/kg/day (females). 35 A TD 50 of 0.819 mg/kg/day (CI 0.44–1.6) was calculated for the predominant tumor site (nasal cavity [12/15 males and 10/14 females]) using the more sensitive sex. An untreated control group was not included in the study; therefore, taking a conservative approach, a background tumor incidence of 0 in 15 was assumed for purposes of supporting the calculation.…”
Section: Resultsmentioning
confidence: 99%
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“…The carcinogenicity of 3-hydroxy- N -nitrosopiperidine was evaluated in rats (15 males, 14 females) after administration via drinking water for 36 weeks (total study duration 50 weeks) resulting in adjusted daily doses of 2.38 (males) and 3.40 mg/kg/day (females). 35 A TD 50 of 0.819 mg/kg/day (CI 0.44–1.6) was calculated for the predominant tumor site (nasal cavity [12/15 males and 10/14 females]) using the more sensitive sex. An untreated control group was not included in the study; therefore, taking a conservative approach, a background tumor incidence of 0 in 15 was assumed for purposes of supporting the calculation.…”
Section: Resultsmentioning
confidence: 99%
“…There was one carcinogenicity study reported in the literature for 1-nitrosopiperidine-4-one, where the N -nitrosamine was administered daily (5 days/week) in drinking water to Sprague–Dawley rats for 36 weeks with a total study duration of 60 weeks. 35 The total cumulative administered dose of 1-nitrosopiperidin-4-one was 3.2 mmol, with corresponding adjusted daily doses in male and female rats of 1.95 and 2.80 mg/kg/day, respectively ( Table S5 ). Both male (14/15) and female (14/15) rats developed adenocarcinomas of the nasal cavity, which was the most sensitive tumor site.…”
Section: Resultsmentioning
confidence: 99%
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“…Nitroso-3-hydroxypiperidine (56u) and nitroso-4-hydroxypiperidine (56t) are carcinogens of potency approximately equal to 56 in rats. Like 56t, 56u induces tumors of the esophagus and nasal mucosa, 333 but 56t also induces many liver tumors, especially in fcmale rats [139]. Thc ketone, nitroso-4-piperidone (56s), like the alcohol 56t gives rise only to tumors of the nasal cavity and liver in SpragueDawley rats [139], but in Fischer 344 rats 56s induces tumors of the liver and esophagus, and is somewhat less potent than 56 [140].…”
Section: Effects Of Substituenl~ In Cyclic Nitrosarninesmentioning
confidence: 99%
“…Like 56t, 56u induces tumors of the esophagus and nasal mucosa, 333 but 56t also induces many liver tumors, especially in fcmale rats [139]. Thc ketone, nitroso-4-piperidone (56s), like the alcohol 56t gives rise only to tumors of the nasal cavity and liver in SpragueDawley rats [139], but in Fischer 344 rats 56s induces tumors of the liver and esophagus, and is somewhat less potent than 56 [140]. Nitroso-3-methyl-4-piperidone (56v) is considerably more potent than 56s, but not more potent than 56, and induces only tumors of the esophagus and tongue, but no liver tumors [140].…”
Section: Effects Of Substituenl~ In Cyclic Nitrosarninesmentioning
confidence: 99%