NTP toxicology and carcinogenesis studies of trans-cinnamaldehyde (CAS No. 14371-10-9) in F344/N rats and B6C3F1 mice (feed studies).

Q4 Medicine

National Toxicology Program technical report series Pub Date : 2004-02-01

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Genetic toxicology studies were conducted in Salmonella typhimurium, cultured Chinese hamster ovary cells, Drosophila melanogaster, and mouse peripheral blood erythrocytes. 3-MONTH STUDY IN RATS: Groups of 10 male and 10 female F344/N rats were fed diets containing 4,100, 8,200, 16,500, or 33,000 ppm microencapsulated trans-cinnamaldehyde (equivalent to average daily doses of approximately 275, 625, 1,300, or 4,000 mg trans-cinnamaldehyde/kg body weight to males and 300, 570, 1,090, or 3,100 mg/kg to females) for 3 months. Additional groups of 10 male and 10 female rats received untreated feed (untreated controls) or feed containing placebo microcapsules (vehicle controls). All rats survived to the end of the study. Mean body weights of all exposed groups of males and 16,500 and 33,000 ppm females were significantly less than those of the vehicle controls, and 33,000 ppm males lost weight during the study. Feed consumption by exposed groups of males and females was less than that by the vehicle controls throughout the study. Clinical chemistry results of these studies indicated that trans-cinnamaldehyde administration, at the doses selected, induced an increase in serum bile acid concentration that suggests a hepatic effect in both male and female rats. Gross lesions observed at necropsy included multifocal to diffuse white nodules of the forestomach mucosa in 8,200 ppm or greater males and females. Increased incidences of nonneoplastic lesions of the forestomach included squamous epithelial hyperplasia in 8,200 ppm or greater males and females and chronic active inflammation in 33,000 ppm males and 16,500 and 33,000 ppm females. 3-MONTH STUDY IN MICE: Groups of 10 male and 10 female B6C3F1 mice were fed diets containing 4,100, 8,200, 16,500, or 33,000 ppm microencapsulated trans-cinnamaldehyde (equivalent to average daily doses of approximately 650, 1,320, 2,550, and 5,475 mg/kg to males and 625, 1,380, 2,680, and 5,200 mg/kg to females) for 3 months. Additional groups of 10 male and 10 female mice received untreated feed (untreated controls) or feed containing placebo microcapsules (vehicle controls). One vehicle control male, one 4,100 ppm male, and one 33,000 ppm male died during the first week of the study due to inanition that resulted from difficulty with the feeder. Five 16,500 ppm and eight 33,000 ppm male mice died during weeks 2 and 3 due to unpalatability of the dosed feed. Mean body weights of all exposed groups of males and of females exposed to 8,200 ppm or greater were significantly less than those of the vehicle controls. Feed consumption by 16,500 and 33,000 ppm mice was less than that by the vehicle controls during weeks 1 and 2. The incidence of squamous epithelial hyperplasia of the forestomach mucosa in 33,000 ppm females was significantly increased, and olfactory epithelial degeneration of the nasal cavity occurred in 16,500 and 33,000 ppm males and females. 2-YEAR STUDY IN RATS: Groups of 50 male and 50 female F344/N rats were fed diets containing 1,000, 2,100, or 4,100 ppm microencapsulated trans-cinnamaldehyde for 2 years. Additional groups of 50 male and 50 female rats received untreated feed (untreated controls) or feed containing placebo microcapsules (vehicle controls). Dietary concentrations of 1,000, 2,100, or 4,100 ppm delivered average daily doses of approximately 50, 100, or 200 mg/kg to males and females. Survival of 4,100 ppm males was greater than that of the vehicle controls. Mean body weights of 4,100 ppm males and females were generally less than those of the vehicle controls throughout the study. Feed consumption by 2,100 and 4,100 ppm males and 4,100 ppm females was less than that by the vehicle controls at the beginning and end of the study. There were no neoplasms or nonneoplastic lesions that were attributed to exposure to trans-cinnamaldehyde. 2-YEAR STUDY IN MICE: Groups of 50 male and 50 female B6C3F1 mice were fed diets containing 1,000, 2,100, or 4,100 ppm microencapsulated trans-cinnamaldehyde for 2 years. Additional groups of 50 male and 50 female mice received untreated feed (untreated controls) or feed containing placebo microcapsules (vehicle controls). Dietary concentrations of 1,000, 2,100, or 4,100 ppm delivered average daily doses of approximately 125, 270, or 550 mg/kg to males and females. Survival of males in the 2,100 ppm group was less than that of the vehicle control group. Mean body weights of 2,100 and 4,100 ppm males and females were generally less than those of the vehicle controls throughout the study, and mean body weights of 1,000 ppm males were less after week 74. Feed consumption by exposed mice was similar to that by the vehicle controls. The incidences of olfactory epithelial pigmentation in 4,100 ppm males and in 2,100 and 4,100 females were significantly greater than those in vehicle controls. There were no neoplasms that were attributed to exposure to trans-cinnamaldehyde.Genetic toxicology: trans-cinnamaldehyde was mutagenic in S. typhimurium strain TA100 in the presence of induced mouse liver S9 activation enzymes only. All other strain and activation combinations, including the standard rat and hamster derived liver S9 fractions yielded negative results. trans-cinnamaldehyde induced sister chromatid exchanges in Chinese hamster ovary cells with and without induced rat liver S9 activation. No significant increase in the frequency of chromosomal aberrations occurred in Chinese hamster ovary cells cultured with trans-cinnamaldehyde, with or without induced rat liver S9. In tests for induction of germ cell genetic damage in male Drosophila melanogaster, trans-cinnamaldehyde induced a significant increase in the frequency of sex-linked recessive lethal mutations when administered by abdominal injection; however, no induction of reciprocal translocations occurred in germ cells of treated males. No increase in the frequency of micronucleated erythrocytes was observed in peripheral blood of male or female mice administered trans-cinnamaldehyde in dosed feed for 3 months.Conclusions: Under the conditions of this 2-year feed study, there was no evidence of carcinogenic activity of transcinnamaldehyde in male or female F344/N rats exposed to 1,000, 2,100, or 4,100 ppm. There was no evidence of carcinogenic activity of trans-cinnamaldehyde in male or female B6C3F1 mice exposed to 1,000, 2,100, or 4,100 ppm. 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Abstract

Unlabelled: Cinnamaldehyde is used in foods, beverages, medical products, perfumes, cosmetics, soaps, detergents, creams, and lotions. Cinnamaldehyde has been used as a filtering agent and a rubber reinforcing agent and is used as a brightener in electroplating processes, as an animal repellent, as an insect attractant, and as an antifungal agent. trans-cinnamaldehyde was nominated for study by the Food and Drug Administration based on its widespread use as a flavor and fragrance ingredient and its structural similarity to cinnamyl anthranilate and 3,4,5-trimethoxy cinnamaldehyde, two known rodent carcinogens. Male and female F344/N rats and B6C3F1 mice were exposed to trans-cinnamaldehyde (at least 95% pure) in feed for 3 months or 2 years. Genetic toxicology studies were conducted in Salmonella typhimurium, cultured Chinese hamster ovary cells, Drosophila melanogaster, and mouse peripheral blood erythrocytes. 3-MONTH STUDY IN RATS: Groups of 10 male and 10 female F344/N rats were fed diets containing 4,100, 8,200, 16,500, or 33,000 ppm microencapsulated trans-cinnamaldehyde (equivalent to average daily doses of approximately 275, 625, 1,300, or 4,000 mg trans-cinnamaldehyde/kg body weight to males and 300, 570, 1,090, or 3,100 mg/kg to females) for 3 months. Additional groups of 10 male and 10 female rats received untreated feed (untreated controls) or feed containing placebo microcapsules (vehicle controls). All rats survived to the end of the study. Mean body weights of all exposed groups of males and 16,500 and 33,000 ppm females were significantly less than those of the vehicle controls, and 33,000 ppm males lost weight during the study. Feed consumption by exposed groups of males and females was less than that by the vehicle controls throughout the study. Clinical chemistry results of these studies indicated that trans-cinnamaldehyde administration, at the doses selected, induced an increase in serum bile acid concentration that suggests a hepatic effect in both male and female rats. Gross lesions observed at necropsy included multifocal to diffuse white nodules of the forestomach mucosa in 8,200 ppm or greater males and females. Increased incidences of nonneoplastic lesions of the forestomach included squamous epithelial hyperplasia in 8,200 ppm or greater males and females and chronic active inflammation in 33,000 ppm males and 16,500 and 33,000 ppm females. 3-MONTH STUDY IN MICE: Groups of 10 male and 10 female B6C3F1 mice were fed diets containing 4,100, 8,200, 16,500, or 33,000 ppm microencapsulated trans-cinnamaldehyde (equivalent to average daily doses of approximately 650, 1,320, 2,550, and 5,475 mg/kg to males and 625, 1,380, 2,680, and 5,200 mg/kg to females) for 3 months. Additional groups of 10 male and 10 female mice received untreated feed (untreated controls) or feed containing placebo microcapsules (vehicle controls). One vehicle control male, one 4,100 ppm male, and one 33,000 ppm male died during the first week of the study due to inanition that resulted from difficulty with the feeder. Five 16,500 ppm and eight 33,000 ppm male mice died during weeks 2 and 3 due to unpalatability of the dosed feed. Mean body weights of all exposed groups of males and of females exposed to 8,200 ppm or greater were significantly less than those of the vehicle controls. Feed consumption by 16,500 and 33,000 ppm mice was less than that by the vehicle controls during weeks 1 and 2. The incidence of squamous epithelial hyperplasia of the forestomach mucosa in 33,000 ppm females was significantly increased, and olfactory epithelial degeneration of the nasal cavity occurred in 16,500 and 33,000 ppm males and females. 2-YEAR STUDY IN RATS: Groups of 50 male and 50 female F344/N rats were fed diets containing 1,000, 2,100, or 4,100 ppm microencapsulated trans-cinnamaldehyde for 2 years. Additional groups of 50 male and 50 female rats received untreated feed (untreated controls) or feed containing placebo microcapsules (vehicle controls). Dietary concentrations of 1,000, 2,100, or 4,100 ppm delivered average daily doses of approximately 50, 100, or 200 mg/kg to males and females. Survival of 4,100 ppm males was greater than that of the vehicle controls. Mean body weights of 4,100 ppm males and females were generally less than those of the vehicle controls throughout the study. Feed consumption by 2,100 and 4,100 ppm males and 4,100 ppm females was less than that by the vehicle controls at the beginning and end of the study. There were no neoplasms or nonneoplastic lesions that were attributed to exposure to trans-cinnamaldehyde. 2-YEAR STUDY IN MICE: Groups of 50 male and 50 female B6C3F1 mice were fed diets containing 1,000, 2,100, or 4,100 ppm microencapsulated trans-cinnamaldehyde for 2 years. Additional groups of 50 male and 50 female mice received untreated feed (untreated controls) or feed containing placebo microcapsules (vehicle controls). Dietary concentrations of 1,000, 2,100, or 4,100 ppm delivered average daily doses of approximately 125, 270, or 550 mg/kg to males and females. Survival of males in the 2,100 ppm group was less than that of the vehicle control group. Mean body weights of 2,100 and 4,100 ppm males and females were generally less than those of the vehicle controls throughout the study, and mean body weights of 1,000 ppm males were less after week 74. Feed consumption by exposed mice was similar to that by the vehicle controls. The incidences of olfactory epithelial pigmentation in 4,100 ppm males and in 2,100 and 4,100 females were significantly greater than those in vehicle controls. There were no neoplasms that were attributed to exposure to trans-cinnamaldehyde.

Genetic toxicology: trans-cinnamaldehyde was mutagenic in S. typhimurium strain TA100 in the presence of induced mouse liver S9 activation enzymes only. All other strain and activation combinations, including the standard rat and hamster derived liver S9 fractions yielded negative results. trans-cinnamaldehyde induced sister chromatid exchanges in Chinese hamster ovary cells with and without induced rat liver S9 activation. No significant increase in the frequency of chromosomal aberrations occurred in Chinese hamster ovary cells cultured with trans-cinnamaldehyde, with or without induced rat liver S9. In tests for induction of germ cell genetic damage in male Drosophila melanogaster, trans-cinnamaldehyde induced a significant increase in the frequency of sex-linked recessive lethal mutations when administered by abdominal injection; however, no induction of reciprocal translocations occurred in germ cells of treated males. No increase in the frequency of micronucleated erythrocytes was observed in peripheral blood of male or female mice administered trans-cinnamaldehyde in dosed feed for 3 months.

Conclusions: Under the conditions of this 2-year feed study, there was no evidence of carcinogenic activity of transcinnamaldehyde in male or female F344/N rats exposed to 1,000, 2,100, or 4,100 ppm. There was no evidence of carcinogenic activity of trans-cinnamaldehyde in male or female B6C3F1 mice exposed to 1,000, 2,100, or 4,100 ppm. Exposure to trans-cinnamaldehyde resulted in olfactory epithelial pigmentation in male and female mice.

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反式肉桂醛(CAS No. 14371-10-9)在F344/N大鼠和B6C3F1小鼠(饲料研究)中的NTP毒理学和致癌作用研究。

未标示:肉桂醛用于食品、饮料、医疗产品、香水、化妆品、肥皂、洗涤剂、面霜和乳液。肉桂醛已被用作过滤剂和橡胶增强剂，在电镀过程中用作光亮剂，作为动物驱避剂，作为昆虫引诱剂，作为抗真菌剂。反式肉桂醛被美国食品和药物管理局提名为研究对象，因为它被广泛用作香料和香料成分，而且它的结构与两种已知的啮齿动物致癌物肉桂酰苯甲酸酯和3,4,5-三甲氧基肉桂醛相似。雄性和雌性F344/N大鼠和B6C3F1小鼠分别暴露于饲料中的反式肉桂醛(纯度至少为95%)3个月或2年。对鼠伤寒沙门菌、培养的中国仓鼠卵巢细胞、黑腹果蝇和小鼠外周血红细胞进行遗传毒理学研究。3个月的大鼠研究:每组10只雄性和10只雌性F344/N大鼠饲喂含有4,100、8,200、16,500或33,000 ppm微胶囊反式肉桂醛的饲料(相当于平均每日剂量约275、625、1,300或4,000 mg/kg体重的雄性和300、570、1,090或3,100 mg/kg体重的雌性)3个月。另外每组10只雄性和10只雌性大鼠分别饲喂未经处理的饲料(未经处理的对照组)或含有安慰剂微胶囊的饲料(对照)。所有的老鼠都活到了研究结束。所有暴露在浓度为16500 ppm和33000 ppm的人群中，男性的平均体重明显低于对照组，而33000 ppm的男性在研究期间体重有所减轻。在整个研究过程中，雄性和雌性暴露组的饲料消耗量低于车辆对照组。这些研究的临床化学结果表明，在选择的剂量下，反式肉桂醛给药诱导血清胆汁酸浓度的增加，这表明在雄性和雌性大鼠中都有肝脏作用。尸检中观察到的大体病变包括前胃黏膜的多灶性弥漫性白色结节，浓度为8200ppm或更高。前胃非肿瘤性病变的发病率增加，包括8200 ppm或更高的男性和女性的鳞状上皮增生，以及33000 ppm的男性和16500 ppm和33000 ppm的女性的慢性活动性炎症。3个月的小鼠研究:每组10只雄性和10只雌性B6C3F1小鼠被喂食含有4,100、8,200、16,500或33,000 ppm微胶囊反式肉桂醛的饮食(相当于雄性的平均日剂量约为650、1,320、2,550和5,475 mg/kg，雌性为625、1,380、2,680和5,200 mg/kg)，为期3个月。另外每组10只雄性和10只雌性小鼠分别饲喂未经处理的饲料(未经处理的对照组)或含有安慰剂微胶囊的饲料(对照)。1只对照雄鼠、1只ppm含量为4100的雄鼠和1只ppm含量为33000的雄鼠在研究的第一周内死亡，原因是喂食器喂食困难导致的缺氧。5只浓度为16500 ppm和8只浓度为33000 ppm的雄性小鼠在第2周和第3周死亡，原因是加了剂量的饲料不好吃。暴露于8200ppm或更高浓度的所有男性和女性暴露组的平均体重明显低于车辆控制组。在第1周和第2周，16500和33,000 ppm小鼠的饲料消耗量低于车辆对照组。33,000 ppm的女性前胃粘膜鳞状上皮增生的发生率显著增加，16,500和33,000 ppm的男性和女性发生鼻腔嗅上皮变性。为期2年的大鼠研究:每组50只雄性和50只雌性F344/N大鼠分别饲喂含有1,000、2,100或4,100 ppm微胶囊反式肉桂醛的饲料2年。另外50只雄性和50只雌性大鼠分别饲喂未经处理的饲料(未经处理的对照组)或含有安慰剂微胶囊的饲料(对照)。膳食浓度为1,000、2,100或4,100 ppm时，男性和女性的平均日剂量约为50、100或200 mg/kg。4100 ppm雄虫的存活率高于对照的雄虫。在整个研究过程中，4100 ppm的男性和女性的平均体重通常低于车辆对照组。在研究开始和结束时，2100 ppm和4100 ppm的雄性和4100 ppm的雌性的饲料消耗低于车辆对照组。没有肿瘤或非肿瘤性病变归因于暴露于反式肉桂醛。为期2年的小鼠研究:每组50只雄性和50只雌性B6C3F1小鼠被喂食含有1,000、2,100或4,100 ppm微胶囊反式肉桂醛的饮食2年。另一组50只雄性和50只雌性小鼠接受未经处理的饲料(未经处理的对照组)或含有安慰剂微胶囊的饲料(对照)。膳食浓度为1000、2100或4100 ppm时，男性和女性的平均日剂量约为125、270或550 mg/kg。2100 ppm组雄性的存活率低于载体对照组。在整个研究过程中，2100 ppm和4100 ppm的男性和女性的平均体重通常低于车辆对照组，而1000 ppm的男性在74周后的平均体重更轻。暴露小鼠的饲料消耗量与对照组相似。嗅觉上皮色素沉着的发生率在4,100 ppm的男性和2,100和4,100女性显著高于对照车辆。没有肿瘤归因于暴露于反式肉桂醛。遗传毒理学:反式肉桂醛仅在小鼠肝脏S9激活酶诱导下对鼠伤寒沙门氏菌TA100具有诱变作用。所有其他菌株和激活组合，包括标准大鼠和仓鼠衍生的肝脏S9组分均为阴性结果。反式肉桂醛诱导大鼠肝脏S9激活和未诱导大鼠卵巢细胞姐妹染色单体交换。经反式肉桂醛培养的中国仓鼠卵巢细胞，不论有无诱导大鼠肝脏S9，染色体畸变发生率均无显著增加。在诱导雄性黑腹果蝇生殖细胞遗传损伤的试验中，通过腹腔注射给药，反式肉桂醛诱导性别连锁隐性致死突变的频率显著增加;然而，在处理过的雄性生殖细胞中没有发生相互易位的诱导。给药3个月后，雌雄小鼠外周血微核红细胞数量均未见增加。结论:在这项为期2年的饲料研究条件下，暴露于1,000、2,100或4,100 ppm的雄性或雌性F344/N大鼠中，没有证据表明跨肉桂醛具有致癌活性。在暴露于1,000、2,100或4,100 ppm浓度的雄性或雌性B6C3F1小鼠中，没有证据表明反式肉桂醛具有致癌活性。暴露于反式肉桂醛导致雄性和雌性小鼠嗅觉上皮色素沉着。

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来源期刊

National Toxicology Program technical report series Medicine-Medicine (all)

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0.30

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0.00%

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