Toxic effects of 4‐methylthio‐3‐butenyl isothiocyanate (Raphasatin) in the rat urinary bladder without genotoxicity

Toxic effects of 4‐methylthio‐3‐butenyl isothiocyanate (Raphasatin) in the rat urinary bladder without genotoxicity

We recently reported that 4‐methylthio‐3‐butenyl isothiocyanate (MTBITC) exerts chemopreventive effects on the rat esophageal carcinogenesis model at a low dose of 80 ppm in a diet. In contrast, some isothiocyanates (ITCs) have been reported to cause toxic effects, promotion activity, and/or carcino...

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Veröffentlicht in:Journal of applied toxicology 2017-04, Vol.37 (4), p.485-494
Hauptverfasser: Suzuki, Isamu, Cho, Young‐Man, Hirata, Tadashi, Toyoda, Takeshi, Akagi, Jun‐ichi, Nakamura, Yasushi, Sasaki, Azusa, Nakamura, Takako, Okamoto, Shigehisa, Shirota, Koji, Suetome, Noboru, Nishikawa, Akiyoshi, Ogawa, Kumiko
Format: Artikel
Sprache:eng
Schlagworte:
4‐methylthio‐3‐butenyl isothiocyanate
Animals
Anticarcinogenic Agents - toxicity
Bladder
Bone Marrow Cells - drug effects
DNA Damage
Eating - drug effects
Esophageal cancer
genotoxicity
Histopathology
Isothiocyanates - toxicity
Male
Mutagenicity Tests
Mutagens - toxicity
Organ Size - drug effects
phenethyl isothiocyanate
Raphasatin
Rats
Rats, Inbred F344
Rodents
Toxicity
Urinary Bladder - drug effects
Urinary Bladder - pathology
Urinary Bladder Diseases - chemically induced
Urinary Bladder Diseases - genetics
Urinary Bladder Diseases - pathology
urinary bladder toxicity
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Zusammenfassung:We recently reported that 4‐methylthio‐3‐butenyl isothiocyanate (MTBITC) exerts chemopreventive effects on the rat esophageal carcinogenesis model at a low dose of 80 ppm in a diet. In contrast, some isothiocyanates (ITCs) have been reported to cause toxic effects, promotion activity, and/or carcinogenic potential in the urinary bladder of rats. In the present study, we investigated whether MTBITC had toxic effects in the urinary bladder similar to other ITCs, such as phenethyl ITC (PEITC). First, to examine the early toxicity of MTBITC, rats were fed a diet supplemented with 100, 300 or 1000 ppm MTBITC for 14 days. Treatment with 1000 ppm MTBITC caused increased organ weights and histopathological changes in the urinary bladder, producing lesions similar to those of 1000 ppm PEITC. In contrast, rats treated with 100 or 300 ppm MTBITC showed no signs of toxicity. Additionally, we performed in vivo genotoxicity studies to clarify whether MTBITC may exhibit a carcinogenic potential through a genotoxic mechanism in rats. Rats were treated with MTBITC for 3 days at doses of 10, 30 or 90 mg kg−1 body weight by gavage, and comet assays in the urinary bladder and micronucleus assays in the bone marrow were performed. No genotoxic changes were observed after treatment with MTBITC at all doses. Overall, these results suggested that the effects of MTBITC in the rat urinary bladder are less than those of PEITC, but that MTBITC could have toxic effects through a nongenotoxic mechanism in the urinary bladder of rats at high doses. Copyright © 2016 John Wiley & Sons, Ltd. We investigated whether 4‐methylthio‐3‐butenyl isothiocyanate (MTBITC), which has known to have chemopreventive effects on rat carcinogenesis at a dose of 80 ppm in the diet, exhibited toxic effects or in vivo genotoxicity in the urinary bladder of rats. We found that treatment with 1000 ppm MTBITC caused non‐genotoxic effects in the urinary bladder, whereas 100 or 300 ppm MTBITC had no toxic effects.
ISSN:0260-437X
1099-1263
DOI:10.1002/jat.3384