ABSTRACT
OBJECTIVE: The study presents the results of a 90-day safety assessment of rats fed with four varieties of soybeans, BRS 245 RR and BRS Valiosa RR (transgenic), BRS 133 and MG BR46 Conquista (non-transgenic). METHODS: Diets were prepared by incorporating toasted soybean flour to a commercial diet at 1%, 10% or 20% weight In the in vivo experimental the rats' body weight, body weight gain, food consumption, number of aberrant crypt foci, oxidative stress biomarkers, urea and creatinine levels were analyzed and compared between experimental groups, as well as histopathological observations (digestive tract, liver, kidneys). RESULTS: The results indicate that glyphosate-tolerant soy varieties neither induce nor prevent aberrant crypt foci induction, nor do their conventional counterparts. Similarly, none of the four soybean varieties tested induced changes in the digestive tract, liver or kidney. Serum biochemical parameters were also unchanged. CONCLUSION: The consumption of both, conventional and transgenic soybeans, were insufficient to ameliorate dimethylhydrazine-induced oxidative stress.
OBJETIVO: Este estudo apresenta os resultados de um experimento de 90 dias com o objetivo de avaliar a segurança de quatro variedades de grãos de soja: BRS 245 RR e BRS Valiosa RR (transgênicas), BRS 133 e MG BR46 Conquista (não transgênicas). MÉTODOS: As dietas foram preparadas incorporando farinha de grãos de soja à dieta comercial (FRI-LAB Ratos II) a 1%, 10% ou 20% m/m. O peso corpóreo dos animais, o ganho de peso, o consumo de dieta, o número de focos de criptas aberrantes e os níveis de marcadores de estresse oxidativo, de creatinina e de ureia foram comparados entre os grupos experimentais, assim como as observações histopatológicas (trato digestivo, fígado e rins). RESULTADOS: Os resultados indicaram que as variantes glifosato-tolerantes não induziram ou preveniram a indução de focos de criptas aberrantes, assim como suas parentais convencionais. Similarmente, nenhuma das quatro variedades de grãos de soja testadas induziu alterações no trato digestivo, no fígado e nos rins. Os parâmetros bioquímicos do soro permaneceram também inalterados. CONCLUSÃO: Tanto o consumo de grãos de soja convencionais quanto o de transgênicos foram ineficazes para melhorar os níveis de estresse oxidativo induzidos pela dimetilhidrazina.
ABSTRACT
Colorectal cancer (CRC) is one of the leading causes of cancer death in western countries or in the developed countries. Zinc intake has been associated with decreased risk of CRC. We investigated the effect of zinc on the formation of colonic aberrant crypt foci (ACF) induced by azoxymethane followed by dextran sodium sulfate in mice. Five-week old ICR mice were fed with the different zinc levels (0.01, 0.1, 1 ppm) for 12 weeks. The numbers of ACF were measured in the colonic mucosa. The ACF number of HZn group was significantly low compared with LZn group or MZn group. Cytosolic superoxide dismutase activity was the highest in HZn group, while thiobarbituric acid reactive substance level for lipid peroxidation was the highest in LZn group. There was no difference in number of PCNA-positive proliferative cells among the groups. TUNEL-positive apoptotic cells were increased in HZn group compared with LZn group. The HZn group exhibited a decrease of beta-catenin immunostaining areas compared with the LZn or MZn group. These findings indicate that dietary zinc might exert a protecting effect against colon carcinogenesis by inhibiting the development of ACF in the mice.
Subject(s)
Animals , Mice , Aberrant Crypt Foci , Azoxymethane , beta Catenin , Colon , Colorectal Neoplasms , Cytosol , Developed Countries , Dextrans , Lipid Peroxidation , Mice, Inbred ICR , Mucous Membrane , Sodium , Sulfates , Superoxide Dismutase , Thiobarbiturates , ZincABSTRACT
We investigated the effect of zinc on the formation of colonic aberrant crypt foci induced by azoxymethane (AOM) followed by dextran sodium sulfate (DSS) in mice with high iron diet (HFe; 450 ppm iron). Six-week old ICR mice were fed on high iron diets with combination of three different levels of zinc in diets, low-zinc (LZn; 0.01 ppm), medium-zinc (MZn; 0.1 ppm), and high-zinc (HZn; 1 ppm) for 12 weeks. Animals were received weekly intraperitoneal injections of AOM (10 mg/kg B.W. in saline) for 3 weeks followed by 2% DSS (molecular weight 36,000~50,000) in the drinking water for a week. To confirm the iron storage in the body, the hepatic iron concentration has been determine chemically and compared with histological assessment visualized by Prussian blue reaction. Aberrant crypt (AC) and aberrant crypt foci (ACF) were analyzed in the colonic mucosa of mouse fed high dietary iron. Superoxide dismutase (SOD) activity and thiobarbituric acid-reactive substances (TBARS) level were also investigated. Apoptosis in the preneoplastic lesion was determined by terminal deoxynucleotidyl transferase-mediated dUTP nickend labeling (TUNEL). In addition, immunohistochemistry of beta-catenin was also performed on the mucous membrane of colon. The number of large ACF (> or = 4 AC/ACF), which possess greater tumorigenic potential, was significantly lower in MZn and HZn groups compared with LZn group. Cytosolic SOD activity in the liver was significantly higher in HZn group compared with LZn group. Hepatic MDA level was decreased significantly in HZn group compared with MZn and LZn groups. Apoptotic index was significantly higher in HZn group. Taken together, these findings indicate that dietary zinc might exert a protective effect against colonic preneoplastic lesion induced by AOM/DSS in ICR mice with high iron status, and suggest that dietary supplement of zinc might play a role in suppressing colon carcinogenesis in mice.
Subject(s)
Animals , Mice , Aberrant Crypt Foci , Apoptosis , Azoxymethane , beta Catenin , Colon , Cytosol , Dextrans , Diet , Dietary Supplements , Drinking Water , Ferrocyanides , Immunohistochemistry , Injections, Intraperitoneal , Iron , Iron Overload , Iron, Dietary , Liver , Mice, Inbred ICR , Mucous Membrane , Prussian Blue Reaction , Sodium , Sulfates , Superoxide Dismutase , ZincABSTRACT
BACKGROUND/AIMS: The purpose of this study was to investigate the malignant potential of aberrant crypt foci (ACF) by measuring the multiplicity of crypts and lectin expression in the early and late stages of 1,2-dimethylhydrazine (DMH)-induced colon carcinogenesis. METHODS: Six-week-old Wistar rats were injected subcutaneously with DMH for 27 weeks. We classified ACF according to the number of crypts per ACF as a few crypts ( or =4 crypts, NC ACF). Immunohistochemistry was used to evaluate lectin expression. RESULTS: In the early stage, FC ACF (590/1,902, 31.0%) occurred more frequently than NC ACF (35/449, 7.8%); whereas in the late stage, NC ACF (176/449, 39.2%) occurred more frequently than FC ACF (324/1,902, 17.0%). The number of ACF peaked at 15 to 20 weeks. The ratio of NC/FC ACF increased gradually during carcinogenesis. The expression of both UEA1 and PNA was higher in NC ACF than FC ACF. Lectin expression increased in the late stage compared with the early stage. CONCLUSIONS: The expression of lectin was higher in NC ACF and ACF in the late stage. Therefore, ACF with higher multiplicities in the late stage may have more malignant potential in DMH-induced colon carcinogenesis.
Subject(s)
Animals , Rats , 1,2-Dimethylhydrazine , Aberrant Crypt Foci , Colon , Dimenhydrinate , Immunohistochemistry , Peanut Agglutinin , Rats, WistarABSTRACT
O isoprenóide geraniol (GO) apresentou atividade quimiopreventiva quando administrado continuamente durante as fases de iniciação e pós-iniciação em modelo de carcinogênese experimental de cólon por meio da redução do número de focos de criptas aberrantes (FCAs) totais FCAs ≥ 4 criptas e aumento de apoptose no cólon distal. Dessa forma, optou-se por avaliar os eventuais efeitos de três doses de GO (GO1: 25mg/100g de peso corpóreo [p.c.], G02: 50 mg/100g de p.c. e G03: 100 mg/100g de p.c.) em categorias de lesões pré-neoplásicas (LPNs) induzidas por dimetilhidrazina (DMH) durante a fase de pós-iniciação tardia de modelo de carcinogênese experimental de cólon, caracterizada por apresentar lesões mais avançadas e com alto grau de alterações celulares morfológicas, bioquímicas e moleculares denominadas de displasia. Para isso, analisamos diferentes biomarcadores como: FCAs totais e FCAs < ou ≥ 4 criptas em cólons corados com azul de metileno; focos depletados ou positivos de mucina (FPMs ou FDMs) em cólons corados com azul de toluidina; FCAs convencionais ou displásicos por meio de análise histopatológica em cortes corados com hematoxilina e eosina (HE) e focos positivos ou negativos para beta-catenina (FPBCs ou FNBCs) citoplasmática e/ou nuclear por meio de imunoistoquímica. Além disso, células apoptóticas foram identificadas utilizando-se critérios morfológicos clássicos em FCAs ≥ 4 no cólon distaI e a expressão de genes envolvidos na carcinogênese de cólon foi avaliada por meio de RT-PCR: HMGCoA-redutase na mucosa colônica e K-Ras e c-myc em FCAs microdissecados. Em relação ao grupo controle, foi possível observar que o grupo tratado com a maior dose de GO (G03) reduziu a freqüência de FCAs ≥ 4 criptas e FDMs, além de aumentar a apoptose em FCAs ≥ 4 displásicos no cólon distaI (p ≤ 0,05). Já, em relação aos outros biomarcadores e às expressões de HMGCoA-redutase, K-Ras e c-myc não observamos diferenças estatísticas entre os tratamentos (p > 0,05). A partir desses resultados, podemos concluir que a dose de 100 mg/100 g de p.c. de GO mostrou ser mais interessante do ponto de vista quimiopreventivo com efeitos observados principalmente no cólon distaI, onde há maiores relatos de incidência de adenocarcinomas colônicos, tanto em animais quanto em humanos. Assim, a indução da morte celular programada em FCAs ≥ 4 preferencialmente displásicos poderia representar um mecanismo importante de atuação de G03 na redução da freqüência de FCAs ≥ 4 criptas e de FDMs (também utilizado como marcador de displasia) durante a fase de pós-iniciação tardia de modelo de carcinogênese experimental de cólon
The isoprenoid geraniol (GO) showed chemopreventive activity when administered continuously during the initiation and post-initiation phases in an experimental model of colon carcinogenesis by reducing the number of total aberrant crypt foci (ACF) and ACFs ≥ 4 crypts, as well as increasing apoptosis in the distal colon. We therefore chose to evaluate the effects of three different doses of GO (GO1: 25 mg/100 g body weight [b.w.], GO2: 50 mg/100 g b.w. and GO3: 100 mg/100 g of b.w.) on preneoplastic lesions (PNLs) induced by dimethylhydrazine (DMH) during late post-initiation in an experimental model of colon carcinogenesis that is characterized by more advanced lesions and a higher degree of cellular alterations morphological, biochemical and molecular (dysplasia) than previous models. For this study, we analyzed the following biomarkers: total ACFs, ACFs < 4 crypts, and ACFs ≥ 4 erypts in colons stained with methylene blue; mucin-depleted or mucin-positive foci (MDFs or MPFs) in colons stained with toluidine blue; ACFs, through conventional or dysplastie histopathological analysis of sections stained with hematoxylin and eosin (HE); and cytoplasmic vs. nuclear foci reactivity for beta-catenin (foci positive for beta-eatenin (FPBC) or foci negative for beta catenin (FNBC)) using immunohistochemistry. Additionally, apoptotic cells were identified using classical morphologic criteria in ACFs ≥ 4 crypts in the distal colon, and the expression of several genes involved in colon carcinogenesis was assessed by RT-PCR, including HMG-CoA reductase in the colonic mucosa and K-Ras and c-myc in microdissected ACFs. Relative to the control group, we observed that the group receiving the highest dose of GO (GO3 group) had a reduced frequency of both ACFs ≥ 4 crypts and MDFs and that apoptosis increased in dysplastic ACFs ≥ 4 crypts in the distal colon (p < 0, 05). Expression of HMG-CoA reductase, K-Ras and c-myc did not differ between treatments (p > 0, 05). Based on these results, we conclude that the 100 mg/100 g b.w. dose of GO is the most promising, as it shows evidence of chemopreventive effects mainly in the distal colon, which is a region that is reported to have a higher incidence of colonic adenocarcinomas, both in animaIs and in humans. lnduction of programmed cell death by GO3 in ACFs ≥ 4 specifically dysplastic could represent an important mechanism of action in reducing the frequency of both ACFs ≥ 4 crypts and MDFs during late post-initiation in this experimental model of colon carcinogenesis
Subject(s)
Animals , Rats , Precancerous Conditions , Colonic Neoplasms , Carcinogenesis , Uterine Cervical Dysplasia , ChemopreventionABSTRACT
Indole-3-carbinol (I3C) found in various cruciferous vegetables has been shown to exert anti-carcinogenic activity in several target organs. Our study was conducted to assess the modifying effect of I3C on the development of colon tumor induced by azoxymethane (AOM). Eighty-seven male F344 rats were divided into 5 groups and were treated with AOM followed by I3C 100 or 300 ppm, AOM alone, I3C alone, and non-treatment, respectively. The animals were subcutaneously injected with AOM. Then diet containing I3C were fed to the rats for 37 weeks. All rats were sacrificed at 40 weeks. Liver and kidney weights of rats treated with I3C at doses of 100 or 300 ppm were significantly increased compared to those of the control group. Colonic tumor incidence and multiplicity of rats treated with I3C at doses of 100 and 300 ppm were not significant compared to those of AOM alone group. In the pathological examination, most of tumors were classified with adenoma and adenocarcinoma in the small and large intestine. These results demonstrated that I3C may have not chemopreventive effect on the rat colon carcinogenesis.
Subject(s)
Animals , Humans , Male , Rats , Adenocarcinoma , Adenoma , Azoxymethane , Colon , Diet , Incidence , Indoles , Intestine, Large , Kidney , Liver , Rats, Inbred F344 , Vegetables , Weights and MeasuresABSTRACT
Cancer chemoprevention utilizing food components is attracted because of its easily availability in humans. Bitter melon (<i>Momordica charantia</i>) (BMO) and pomegranate (<i>Punica granatum</i> L.) (PGO) seed oils contain a large amount of conjugated linolenic acid (CLN). In the first we demonstrated that BMO inhibits the development of azoxymethane (AOM)-induced putative precursor lesions for colonic adenocarcinoma in rats. Subsequently, we investigated the modifying effects of dietary administration of BMO or PGO on the development of colonic neoplasms using an animal colon carcinogenesis model initiated with a colon carcinogen AOM. Male F344 rats were given two weekly subcutaneous injections of AOM (20 mg/kg body weight) to induce colonic neoplasms. They were fed with the diets containing 0.01%, 0.1% and 1% BMO or PGO during the entire experimental period (for 32 weeks), starting one week before the first dosing of AOM. At the end of the study, the incidence and multiplicity of colonic adenocarcinoma were reduced in the "AOM+BMO" and "AOM+PGO" groups, when compared with the "gAOM alone" group. The contents of conjugated linoleic acid (CLA: 9<i>c</i>,11<i>t</i>-18:2) in the liver and colonic mucosa of rats fed BMO or PGO were elevated in a dose-dependent manner. Also, dietary BMO or PGO enhanced expression of peroxisome proliferator-activated receptor (PPAR)γ protein in the colonic mucosa. These findings may suggest that BMO or PGO rich in CLN can suppress AOM-induced colon carcinogenesis through the modification of lipid composition in the colon and liver and/or increased expression of PPARγ protein level in the colon mucosa. Our results might provide scientific evidence of an effective dietary chemopreventive approach using BMO and PGO seed oils rich in CLN to cancer chemoprevention, especially colon cancer development.<br>
ABSTRACT
The inhibitory effects of ginseng on the development of 1,2-dimethylhydrazine (DMH)-induced aberrant crypt foci (ACF) in the colon were investigated in rats. Male, 6-week-old rats were injected with DMH once a week for 4 weeks. Rats in Groups 1 and 2 were fed diets containing red and white ginseng, rerspectively, at a dose of 1% for 5 weeks, starting one week before the first treatment of DMH. Animals in Groups 3 and 4 received red or white ginseng for 8 weeks starting after DMH treatment. Group 5 served as a carcinogen control group. Numbers of ACF with at least four crypts were significantly reduced in the colon of Group 2 treated with red ginseng combined with DMH. Moreover, rats were injected with DMH 4 times at one-week intervals. They were also fed diets containing 1% red or white ginseng or the control diet throughout 30 days of the experiment. Treatment with red ginseng resulted in a significant decrease of 5- bromo-2'-deoxyuridine labeling indices in colonic crypts comprising ACF. These findings suggest that dietary administration of red ginseng in combination with DMH suppresses colon carcinogenesis in rats, and the inhibition may be associated, in part, with inhibition of cell proliferation, acting on ACF in the colonic mucosa.