{"title":"Synthetic Musks Fragrances In The AquaticEnvironment: In Vitro Toxicological Studies OfTheir Biotransformation AndPotential Negative Effects","authors":"S. Focardi, C. D. Torre, M. Monti, T. Biagini, I. Corsi","doi":"10.2495/EHR110171","DOIUrl":null,"url":null,"abstract":"The aim of the present study was to investigate the interaction of musk xylene (MX) and Tonalide (AHTN) with CYP1A by looking at gene transcription (cyp1a) and EROD activity in Poeciliopsis lucida hepatoma cell line (PLHC-1). MX and AHTN were studied individually and combined with classical inducer of CYP1A as B(a)P and PCB126. After 24h of exposure a different cytotoxicity has been observed with an LC50 of 35.76μM for AHTN and LC50 123.6μM for MX. After 6h of exposure to MX, a dose-dependent reduction of cyp1a was observed respect to controls. At 24h, the same pattern was observed but with slight induction at the lowest concentration (2μM) and a dose-dependent reduction at the higher concentrations. Co-exposure to MX with B(a)P did not alter cyp1a transcription levels compared to the inducer alone. After 6h AHTN determined a slight induction of cyp1a transcription reaching maximum induction of 2.3 folds respect to controls at 2μM. No modulation of cyp1a transcription was observed after 24h. Co-exposure to AHTN with B(a)P and PCB126 at 6h determined a 55% reduction of cyp1a transcription respect to inducers alone which recovered at 24h. At 24h, MX caused a dose-dependent decrease of EROD activity. No modulation of EROD activity was detectable at 6h and 24h of exposure to AHTN. Co-exposure with both MX and AHTN did not alter EROD activity induced by B(a)P and PCB126. Results suggest different toxicological properties of MX and AHTN toward CYP1A in PLHC-1. MX reduced cyp1a basal transcription but did not alter cyp1a induction by B(a)P and PCB126. This suggests that MX cellular pathway is not mediated by AhR. On Environmental Health and Biomedicine 183 www.witpress.com, ISSN 1743-3525 (on-line) WIT Transactions on Biomedicine and Health, Vol 15, © 2011 WIT Press doi:10.2495/EHR11171 the contrary AHTN did not alter significantly cyp1a basal levels but decreased cyp1a induction by B(a)P and PCB126. A potential role of AHTN as competitive antagonist of AhR could thus be hypothesized.","PeriodicalId":370021,"journal":{"name":"WIT Transactions on Biomedicine and Health","volume":"1 1","pages":"0"},"PeriodicalIF":0.0000,"publicationDate":"2011-07-14","publicationTypes":"Journal Article","fieldsOfStudy":null,"isOpenAccess":false,"openAccessPdf":"","citationCount":"0","resultStr":null,"platform":"Semanticscholar","paperid":null,"PeriodicalName":"WIT Transactions on Biomedicine and Health","FirstCategoryId":"1085","ListUrlMain":"https://doi.org/10.2495/EHR110171","RegionNum":0,"RegionCategory":null,"ArticlePicture":[],"TitleCN":null,"AbstractTextCN":null,"PMCID":null,"EPubDate":"","PubModel":"","JCR":"","JCRName":"","Score":null,"Total":0}
引用次数: 0
水生环境中的合成麝香:生物转化和潜在负面影响的体外毒理学研究
本研究的目的是通过观察luceciliopsis hepatoma细胞株(PLHC-1)的基因转录(CYP1A)和EROD活性,研究麝香二甲苯(MX)和麝香萘啶(AHTN)与CYP1A的相互作用。分别研究MX和AHTN,并与CYP1A经典诱导剂B(a)P和PCB126联合。暴露24小时后,观察到不同的细胞毒性,AHTN的LC50为35.76μM, MX的LC50为123.6μM。暴露于MX 6小时后,与对照组相比,cyp1a呈剂量依赖性减少。在24h,观察到相同的模式,但在最低浓度(2μM)有轻微的诱导,在较高浓度有剂量依赖性的减少。与单独的诱导剂相比,MX与B(a)P共同暴露没有改变cyp1a的转录水平。6h后,AHTN检测到cyp1a转录的轻微诱导,在2μM时达到最大诱导量,是对照的2.3倍。24h后未观察到cyp1a转录的调节。AHTN与B(a)P和PCB126共暴露于6h时,cyp1a转录比单独诱变剂减少55%,并在24h时恢复。24小时时,MX引起EROD活性呈剂量依赖性下降。暴露于AHTN 6h和24h时,没有检测到EROD活性的调节。与MX和AHTN共同暴露对B(a)P和PCB126诱导的EROD活性没有影响。结果表明,MX和AHTN对PLHC-1中CYP1A的毒理学特性不同。MX降低了cyp1a的基础转录,但没有改变B(a)P和PCB126对cyp1a的诱导。这表明MX细胞通路不是由AhR介导的。On Environmental Health and biomedine 183 www.witpress.com, ISSN 1743-3525 (online) WIT Transactions On biomedine and Health, Vol 15,©2011 WIT Press doi:10.2495/EHR11171相反,AHTN没有显著改变cyp1a基础水平,但降低了B(a)P和PCB126对cyp1a的诱导。因此,可以假设AHTN作为AhR的竞争性拮抗剂的潜在作用。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
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