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논문 기본 정보

자료유형
학술저널
저자정보
Ryu, Jae-Chun (Toxicology Laboratory, Doping Control Center, Korea Institute of Scienece and Technology) Kim, Kyung-Ran (Toxicology Laboratory, Doping Control Center, Korea Institute of Scienece and Technology) Kim, Hyun-Joo (Toxicology Laboratory, Doping Control Center, Korea Institute of Scienece and Technology) Ryu, Eun-Kyoung (Toxicology Laboratory, Doping Control Center, Korea Institute of Scienece and Technology) Lee, Soo-Young (Toxicology Laboratory, Doping Control Center, Korea Institute of Scienece and Technology) Jung, Sang-Oun (Toxicology Laboratory, Doping Control Center, Korea Institute of Scienece and Technology) Youn, Ji-Youn (Toxicology Laboratory, Doping Control Center, Korea Institute of Scienece and Technology) Kim, Min-Hee (Toxicology Laboratory, Doping Control Center, Korea Institute of Scienece and Technology) Kwon, Oh-Seung (Toxicology Laboratory, Doping Control Center, Korea Institute of Scienece and Technology)
저널정보
대한약학회 Archives of pharmacal research : a publication of the Pharmaceutical Society of Korea Archives of pharmacal research : a publication of the Pharmaceutical Society of Korea 제19권 제4호
발행연도
1996.1
수록면
251 - 257 (7page)

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초록· 키워드

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The detection of many synthetic chemicals used in industry that may pose a genetic hazard in our environment is subject of great concern at present. In this respect, the genetic toxicity of fenpropathrin ((RS)-.alpha.-cyano-3-phenoxybenzyl-2,2,3,3-tetramethyl cyclopropane carboxylate, CAS No.:39514-41-8), a pyrethroid insecticide, was evaluated in bacterial gene mutation system, chromosome aberration in mammalian cell system and in vivo micronucleus assay with rodents. In bacterial gene mutation assay, no mutagenicity of fenpropathrin (62-$5000\mug/plate$) was observed in Salmonella typhimurium TA 98, 100, 1535 and 1537 both in the absence and in the presence of S-9 metabolic activaton system. In mammalian cell system using chinese hamster lung fibroblast, no clastogenicity of fenpropathrin was also observed both in the absence and in the presence of metabolic activation system in the concentration range of $7-28\mug/ml$. And also, in vivo micronucleus assay using mouse bone marrow cells, fenpropathrin also revealed no mutagenic potential in the dose range of 27-105 mg/kg body weight of fenpropathrin (i.p.). Consequently, no mutagenic potential of fenpropathrin was observed in vitro bacterial, mammalian mutagenicity systems and in vivo micronucleus assay in the dose ranges used in this experiment.

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