Transgenic Rats Carrying Human c‐Ha‐<i>ras</i> Proto‐oncogene Are Highly Susceptible to N‐Nitrosomethylbenzylamine Induction of Esophageal Tumorigenesis

Asamoto, Makoto; Toriyama‐Baba, Hiroyasu; Ohnishi, Takamasa; Naito, Akira; Ota, Tomohiro; Ando, Akira; Ochiya, Takahiro; Tsuda, Hiroyuki

doi:10.1111/j.1349-7006.2002.tb01315.x

Cited by 21 publications

(19 citation statements)

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“…N-nitrosomethylbenzylamine esophageal, 35) and DMBA skin carcinogenesis. 36) We recently showed that the transgenic (Tg) rats have a potential for use in medium-term bioassay models to test for the modifying effects of estrogenic environmental compounds on mammary tumor development.…”

Section: )mentioning

confidence: 99%

“…Most of the tumor cells contained mutated transgene, but not endogenous Hras gene, indicating that activation of the transgene plays an important role in such rapid development of tumors. The animals have also been found to be susceptible to N-butyl-N-(4-hydroxybutyl)nitrosamine urinary bladder, 34) N-nitrosomethylbenzylamine esophageal, 35) and DMBA skin carcinogenesis. 36) We recently showed that the transgenic (Tg) rats have a potential for use in medium-term bioassay models to test for the modifying effects of estrogenic environmental compounds on mammary tumor development.…”

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confidence: 99%

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Possible enhancing effects of atrazine and nonylphenol on 7,12‐dimethylbenz[a]anthracene‐induced mammary tumor development in human c‐Ha‐ras proto‐oncogene transgenic rats

Fukamachi¹,

Han

Kim

et al. 2004

Cancer Science

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Our transgenic (Tg) strain carrying copies of the human c-Ha-ras proto-oncogene is highly susceptible to 7,12-dimethylbenz[a]anthracene (DMBA)-induced mammary carcinogenesis, possibly due to activation of the transgene, and can be used in medium-term bioassay models to test for modifying effects of estrogenic environmental compounds on tumor development. The present study was conducted to assess the influence of dietary feeding of the endocrine disruptors atrazine and nonylphenol on DMBA-induced carcinogenesis in c-Ha-ras Tg rats. Animals of both sexes were given a single oral dose of DMBA (25 mg/kg body weight) at 50 days of age and thereafter received soybean-free diet containing 5, 50 or 500 ppm atrazine, or 10, 25, 100 or 250 ppm nonylphenol. In female Tg rats, atrazine at a dose of 5 ppm increased the incidences of mammary adenomas and adenocarcinomas (P < < < <0.01 and P < < < <0.05), while 50 ppm increased the adenocarcinoma incidence (P < < < <0.05). In males, skin tumor development, in contrast, was significantly decreased at the highest dose. Nonylphenol at 10 ppm increased adenocarcinoma and total mammary tumor multiplicity in female Tg rats (P < < < <0.05), but there was no dose dependence, a significant quadratic dose-response trend rather being observed (P < < < <0.05). In vitro, atrazine did not cause proliferation of MCF-7 cells at any of a range of doses tested. These results suggest that endocrine disruptors may enhance mammary carcinogenesis, but only in a certain limited dose range under the present experimental conditions. The doses applied, moreover, were all extremely high compared to the possible environmental human exposure levels. (Cancer Sci 2004; 95: 404-410) t is well documented that estrogen is an obligatory factor for development of the mammary gland.1, 2) The hormone also plays an important role in both the etiology and treatment of mammary cancer and accumulating evidence indicates that slightly elevated levels of circulating estrogens may predispose to tumorigenesis.3, 4) Exogenous estrogens may similarly increase mammary cancer risk.5-7) This may be of considerable importance, since recently, a number of environmental chemicals impacting on the endocrine system (endocrine disruptors) have been shown to exhibit estrogenic activity, these including triazine derivatives and alkylphenolic compounds.Among the symmetrical triazine-type herbicides, atrazine (6-chloro-N 2 -ethyl-N 4 -isopropyl-1,3,5-triazine-2,4-diamine) is one of the most widely and heavily used herbicides all over the world. It is employed in agriculture as a selective pre-and postemergence agent for annual control of grass and broad-leaved weeds. A number of studies have suggested that atrazine is an endocrine disruptor [8][9][10][11][12][13][14][15] and in female Sprague-Dawley, but not other strains of rats, high doses (50-1000 ppm) in the diet have been found to be associated with an increased incidence and/or an earlier onset of mammary gland tumors. [16][17][18][19][20] Alkylphenol polyethoxylates are the se...

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confidence: 99%

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confidence: 99%

Possible enhancing effects of atrazine and nonylphenol on 7,12‐dimethylbenz[a]anthracene‐induced mammary tumor development in human c‐Ha‐ras proto‐oncogene transgenic rats

Fukamachi¹,

Han

Kim

et al. 2004

Cancer Science

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“…7) In humans, Ki-ras mutations are preferentially found in colon, 8,9) pancreatic duct 10) and bile duct carcinomas, 11) and N-ras mutations are typically seen in myeloid leukemia. 12) We have generated a transgenic rat line, harboring copies of a human c-Ha-ras proto-oncogene (Hras128 rat), and have shown that these animals are highly susceptible to mammary, 13,14) bladder 15) and esophageal 16) carcinogens.…”

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confidence: 99%

Preferential mammary carcinogenic effects of 2‐amino‐1‐methyl‐6‐phenylimidazo[4,5‐b]pyridine (PhIP) in human c‐Ha‐ras proto‐oncogene transgenic rats

et al. 2004

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he Ras family is composed of three members, Harvey Ras, Kirsten Ras and N-Ras, which exhibit mutations at variable frequencies in various human and animal tumors, 1) with involvement appearing to be tissue-specific. 2, 3) For example, with N-methyl-N-nitrosourea (MNU) in experimental animals, Haras mutations are found primarily in mammary tumors, [4][5][6] while colon tumors generally have Ki-ras mutations. 7) In humans, Ki-ras mutations are preferentially found in colon, 8,9) pancreatic duct 10) and bile duct carcinomas, 11) and N-ras mutations are typically seen in myeloid leukemia. 12) We have generated a transgenic rat line, harboring copies of a human c-Ha-ras proto-oncogene (Hras128 rat), and have shown that these animals are highly susceptible to mammary, 13,14) bladder 15) and esophageal 16) carcinogens.Heterocyclic amines found in overcooked foods are both mutagenic and carcinogenic to animals, 17) and 2-amino-1-methyl-6-phenylimidazo [4,5-b]pyridine (PhIP), the most abundant in our daily diet, 18) has been shown to induce primarily colon, mammary and prostate tumors in rats. [19][20][21] PhIP intake in food has also been implicated as an important risk factor in humans 22,23) although further analysis of the interactions between PhIP and relevant macromolecules is required for a full understanding of the carcinogenic processes.Although mutational analyses of tumors induced by PhIP have been conducted, 24) specific molecular targets have yet to be elucidated. One problem is that the relatively weak carcinogenic potential requires the use of long experimental periods for lesion induction. This study was conducted to analyze the susceptibility of Hras128 rats to PhIP, in the hope of overcoming the above problem. We show here that Hras128 rats are in fact highly susceptible to PhIP mammary carcinogenesis, and multiple tumors of various morphological types develop in a short period. Furthermore, they feature mutations of the transgene along with down-regulation of BRCA1. Materials and MethodsAnimals and experimental protocol. Seven-week-old Hras128 rats of both sexes were maintained on basal diet (Oriental MF, Oriental Yeast Co., Ltd. Tokyo) with tap water ad libitum under standard conditions. 13) Seven females and 18 males were treated with PhIP HCl salt (NARD Institute, Osaka), at doses of 100 mg and 80 mg/kg body weight, respectively, by gastric intubation, from 3 to 4 times a week over a 9-week period (total, 8 times in females and 10 times in males). Five female and 20 male Hras128 rats were similarly treated with vehicle (saline). Sacrifice was at week 12 for females and week 30 for males. Seven female and 20 male wild-type littermates were also treated with PhIP, and 8 female and 20 male wild-type littermates received the vehicle (saline).The experiments were conducted according to the "Guidelines for Animal Experiments in the National Cancer Center Japan" promulgated by the Committee for Ethics of Animal Experimentation.Tissue preparation. Immediately after killing of the animals, mammary tumors wer...

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“…These data suggest that mutational activation of the H-ras gene is important for progression of the premalignant lesions to papillomas. Additional evidence in support of this concept is the observation that transgenic rats carrying the human c-Ha-ras proto-oncogene are highly susceptible to the induction of esophageal tumors with NMBA (Asamoto et al, 2002). As has been found in human esophageal tumors, G:C→ A:T transition mutations have been observed in the p53 tumor suppressor gene in ∼30 % of rat esophageal papillomas (Lozano et al, 1994;.…”

Section: Rat Esophageal Tumor Modelmentioning

confidence: 74%

Chemoprevention of esophageal squamous cell carcinoma

Stoner

Wang

Chen

2007

Toxicology and Applied Pharmacology

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Esophageal squamous cell carcinoma (SCC) is responsible for approximately one-sixth of all cancerrelated mortality worldwide. This malignancy has a multifactorial etiology involving several environmental, dietary and genetic factors. Since esophageal cancer has often metastasized at the time of diagnosis, current treatment modalities offer poor survival and cure rates. Chemoprevention offers a viable alternative that could well be effective against the disease. Clinical investigations have shown that primary chemoprevention of this disease is feasible if potent inhibitory agents are identified. The Fischer 344 (F-344) rat model of esophageal SCC has been used extensively to investigate the biology of the disease, and to identify chemopreventive agents that could be useful in human trials. Multiple compounds that inhibit tumor initiation by esophageal carcinogens have been identified using this model. These include several isothiocyanates, diallyl sulfide and polyphenolic compounds. These compounds influence the metabolic activation of esophageal carcinogens resulting in reduced genetic (DNA) damage. Recently, a few agents have been shown to inhibit the progression of preneoplastic lesions in the rat esophagus into tumors. These agents include inhibitors of inducible nitric oxide synthase (iNOS), cyclooxygenase-2 (COX-2), vascular endothelial growth factor (VEGF) and c-Jun [a component of activator protein-1 (AP-1)]. Using a food based approach to cancer prevention, we have shown that freeze-dried berry preparations inhibit both the initiation and promotion/progression stages of esophageal SCC in F-344 rats. These observations have led to a clinical trial in China to evaluate the ability of freeze-dried strawberries to influence the progression of esophageal dysplasia to SCC.

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Transgenic Rats Carrying Human c‐Ha‐ras Proto‐oncogene Are Highly Susceptible to N‐Nitrosomethylbenzylamine Induction of Esophageal Tumorigenesis

Cited by 21 publications

References 26 publications

Possible enhancing effects of atrazine and nonylphenol on 7,12‐dimethylbenz[a]anthracene‐induced mammary tumor development in human c‐Ha‐ras proto‐oncogene transgenic rats

Possible enhancing effects of atrazine and nonylphenol on 7,12‐dimethylbenz[a]anthracene‐induced mammary tumor development in human c‐Ha‐ras proto‐oncogene transgenic rats

Preferential mammary carcinogenic effects of 2‐amino‐1‐methyl‐6‐phenylimidazo[4,5‐b]pyridine (PhIP) in human c‐Ha‐ras proto‐oncogene transgenic rats

Chemoprevention of esophageal squamous cell carcinoma

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