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Toxicity Screening of Bisphenol A Replacement Compounds: Cytotoxicity and mRNA Expression in Primary Hepatocytes of Chicken and Double-Crested Cormorant

机译:双酚的毒性筛选替代化合物:鸡肉和双冠状藻类母孢子细胞中的细胞毒性和mRNA表达

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A market for bisphenol A (BPA) replacement compounds has emerged as a result of restrictions on the use of BPA. Some of these compounds have been detected in the environment; however, little is known about their toxicological properties. In the present study, an avian in vitro toxicogenomic approach was used to compare the effects of 5 BPA alternatives. Cell viability and mRNA expression were compared in primary embryonic hepatocytes of chicken (CEH) and double-crested cormorant (DCEH) exposed to 4,4 '-(propane-2,2-diyl) diphenol (BPA), bis (4-hydroxyphenyl) methane (BPF), bis (3-allyl-4-hydroxyphenyl) sulfone (TGSH), 7-bis (4-hydroxyphenylthio)-3,5-dioxaheptane (DD-70), 2,2-bis (4-hydroxyphenyl) hexafluoropropane (BPAF), and 4-hydroxyphenyl 4-isoprooxyphenylsulfone (BPSIP). Changes in gene expression were determined using 2 polymerase chain reaction (PCR) arrays: 1) species-specific ToxChips that contain genes representing toxicologically relevant pathways, and 2) chicken-specific AestroChip that measures estrogen responsive genes. In CEH and DCEH, BPA alternatives TGSH, DD-70, and BPAF were most cytotoxic. Some of the replacement compounds changed the expression of genes related to xenobiotic metabolism, bile acid, and cholesterol regulation. The rank order based on the number of genes altered on the chicken ToxChip array was TGSH DD-70 BPAF = BPF 17 beta estradiol (E2) BPSIP BPA. On the cormorant ToxChip array, BPSIP altered the greatest number of genes. Based on the chicken AestroChip data, BPSIP and BPF were slightly estrogenic. These results suggest that the replacement compounds have comparable or even greater toxicity than BPA and act via different mechanisms. Environ Toxicol Chem 2021;00:1-11. (c) 2021 Her Majesty the Queen in Right of Canada. Reproduced with the permission of the Minister of Environment and Climate Change Canada.
机译:由于对使用BPA的使用而出现了双酚A(BPA)更换化合物的市场。这些化合物中的一些已经在环境中进行了检测;然而,对其毒理学特性知之甚少。在本研究中,用于比较5 bpa替代品的疗法的体外毒性方法。将细胞活力和mRNA表达在鸡(CEH)的原发性胚胎肝细胞和暴露于4,4' - (丙烷-2,2-二基)二酚(BPA),双(4-羟基苯基) )甲烷(BPF),双(3-烯丙基-4-羟基苯基)砜(TGSH),7-双(4-羟基苯硫基)-3,5-二氧杂丁烷(DD-70),2,2-双(4-羟基苯基),2,2-二苯基)六氟丙烷(BPAF)和4-羟基苯基4-异丙氧基苯基砜(BPSIP)。使用2种聚合酶链反应(PCR)阵列测定基因表达的变化:1)特异性毒素,其含有代表毒理学相关途径的基因,以及2)患雌激素响应基因的鸡特异性含量。在CEH和DCEH中,BPA替代品TGSH,DD-70和BPAF是最多的细胞毒性。一些替代化合物改变了与异蛋白代谢,胆汁酸和胆固醇调节有关的基因的表达。基于鸡肉趾阵列上改变的基因数量的等级顺序是TGSH> DD-70> BPAF = BPF>17β雌二醇(E2)> BPSIP> BPA。在鸬鹚毒素阵列上,BDSIP改变了最多的基因。基于鸡Aestrochip数据,BDSIP和BPF略微雌激素。这些结果表明,替代化合物的毒性比BPA相当或甚至更大的毒性,并通过不同的机制起作用。环境毒素化学2021; 00:1-11。 (c)2021年陛下在加拿大右边的女王。凭借加拿大环境和气候变化部长的许可。

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