Cantón Rocío F, Sanderson J Thomas, Nijmeijer Sandra, Bergman Ake, Letcher Robert J, van den Berg Martin
Institute for Risk Assessment Sciences (IRAS), University of Utrecht, Yalelaan 2, 3508 TD, Utrecht, The Netherlands.
Toxicol Appl Pharmacol. 2006 Oct 15;216(2):274-81. doi: 10.1016/j.taap.2006.05.007. Epub 2006 May 19.
Fire incidents have decreased significantly over the last 20 years due, in part, to regulations requiring addition of flame retardants (FRs) to consumer products. Five major classes of brominated flame retardants (BFRs) are hexabromocyclododecane isomers (HBCDs), tetrabromobisphenol-A (TBBPA) and three commercial mixtures of penta-, octa- and deca-polybrominated diphenyl ether (PBDE) congeners, which are used extensively as commercial FR additives. Furthermore, concentrations of PBDEs have been rapidly increasing during the 1999s in human breast milk and a number of endocrine effects have been reported. We used the H295R human adrenocortical carcinoma cell line to assess possible effects of some of these BFRs (PBDEs and several of their hydroxylated (OH) and methoxylated (CH(3)O) metabolites or analogues), TBBPA and brominated phenols (BPs) on the combined 17alpha-hydroxylase and 17,20-lyase activities of CYP17. CYP17 enzyme catalyzes an important step in sex steroidogenesis and is responsible for the biosynthesis of dehydroepiandrosterone (DHEA) and androstenedione in the adrenals. In order to study possible interactions with BFRs, a novel enzymatic method was developed. The precursor substrate of CYP17, pregnenolone, was added to control and exposed H295R cells, and enzymatic production of DHEA was measured using a radioimmunoassay. In order to avoid pregnenolone metabolism via different pathways, specific chemical inhibitor compounds were used. None of the parent/precursor BFRs had a significant effect (P < 0.05) on CYP17 activity except for BDE-183, which showed significant inhibition of CYP17 activity at the highest concentration tested (10 muM), with no signs of cytotoxicity as measured by mitochondrial toxicity tests (MTT). A strong inhibition of CYP17 activity was found for 6-OH-2,2',4,4'-tetrabromoDE (6-OH-BDE47) with a concentration-dependent decrease of almost 90% at 10 muM, but with a concurrent decrease in cell viability at the higher concentrations. Replacement of the 6-OH group by a 6-CH(3)O group eliminated this cytotoxic effect, but CYP17 activity measured as DHEA production was still significantly inhibited. Other OH- or CH(3)O-PBDE analogues were used to elucidate possible structural properties behind this CYP17 inhibition and associated cytotoxicity, but no distinct structure activity relationship could be determined. These in vitro results indicate that OH and CH(3)O-PBDEs have potential to interfere with CYP17 activity for which the in vivo relevance still has to be adequately determined.
在过去20年里,火灾事故显著减少,部分原因是法规要求在消费品中添加阻燃剂(FRs)。溴化阻燃剂(BFRs)的五大主要类别是六溴环十二烷异构体(HBCDs)、四溴双酚A(TBBPA)以及五溴、八溴和十溴多溴二苯醚(PBDE)同系物的三种商业混合物,它们被广泛用作商业FR添加剂。此外,在20世纪90年代,人母乳中多溴二苯醚的浓度迅速上升,并且已有一些内分泌效应的报道。我们使用H295R人肾上腺皮质癌细胞系来评估其中一些BFRs(多溴二苯醚及其几种羟基化(OH)和甲氧基化(CH₃O)代谢物或类似物)、TBBPA和溴化酚(BPs)对CYP17的17α-羟化酶和17,20-裂解酶联合活性的可能影响。CYP17酶催化性类固醇生成中的一个重要步骤,负责肾上腺中脱氢表雄酮(DHEA)和雄烯二酮的生物合成。为了研究与BFRs可能的相互作用,开发了一种新的酶促方法。将CYP17的前体底物孕烯醇酮添加到对照和暴露的H295R细胞中,并使用放射免疫测定法测量DHEA的酶促产生。为了避免孕烯醇酮通过不同途径代谢,使用了特定的化学抑制剂化合物。除了BDE-183外,母体/前体BFRs均对CYP17活性无显著影响(P < 0.05),BDE-183在最高测试浓度(10 μM)时显示出对CYP17活性的显著抑制,通过线粒体毒性试验(MTT)测量无细胞毒性迹象。发现6-OH-2,2',4,4'-四溴二苯醚(6-OH-BDE47)对CYP17活性有强烈抑制作用,在10 μM时浓度依赖性降低近90%,但在较高浓度时细胞活力同时下降。用6-CH₃O基团取代6-OH基团消除了这种细胞毒性作用,但以DHEA产生量衡量的CYP17活性仍被显著抑制。使用其他OH-或CH₃O-PBDE类似物来阐明这种CYP17抑制和相关细胞毒性背后可能的结构特性,但无法确定明显的构效关系。这些体外结果表明,OH和CH₃O-PBDEs有可能干扰CYP17活性,其体内相关性仍有待充分确定。
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