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双酚类物质 BPA、BPS 和 BPF 代谢研究的最后一块拼图:体外磺化反应动力学。

Last piece in the puzzle of bisphenols BPA, BPS and BPF metabolism: Kinetics of the in vitro sulfation reaction.

机构信息

Faculty of Pharmacy, University of Ljubljana, Ljubljana, Slovenia.

Faculty of Pharmacy, University of Ljubljana, Ljubljana, Slovenia.

出版信息

Chemosphere. 2022 Sep;303(Pt 2):135133. doi: 10.1016/j.chemosphere.2022.135133. Epub 2022 May 27.

Abstract

Bisphenols are endocrine-disrupting chemicals ubiquitously present in the environment, with the consequent exposure to humans. In humans, bisphenols are metabolized to glucuronide and sulfate conjugates. Recent studies indicate that sulfation represents an important bisphenol metabolic pathway for the most vulnerable humans, such as the growing fetus. Our aim was to evaluate sulfation kinetics of commonly detected bisphenols in biological samples: bisphenol A (BPA), bisphenol S (BPS), and bisphenol F (BPF). Furthermore, we evaluated estrogenic agonist potencies and long-term stability of these bisphenol sulfates. BPS and BPF sulfates were prepared by chemical synthesis. Sulfation kinetics of the selected bisphenols were tested in pooled human liver cytosol, as a source for soluble phase II enzymes, including liver sulfotransferases, with quantification by LC-MS/MS. A validated transactivation assay using the hERα-Hela 9903 cell line was used to determine estrogenic agonist potencies. Moreover, BPA, BPS, and BPF sulfate stabilities were examined under various conditions and during storage. In vitro sulfation of BPA and BPS followed Michaelis-Menten kinetics; BPF sulfation followed a substrate inhibition model. Sulfation rates were comparable for these bisphenols, although their K values indicated some large differences in affinities. BPA and BPS sulfates are not hERα agonists. The bisphenol sulfates can be considered stable for at least 2 days under these tested media conditions. These data indicate that bisphenol sulfation is an important route in their biotransformation. Compared to glucuronidation, these bisphenols show slower sulfation rates but similar K values. BPA and BPS metabolic biotransformation by sulfation provides their detoxification as they are without estrogenic activities.

摘要

双酚类物质是环境中普遍存在的内分泌干扰化学物质,人类因此会接触到这些物质。在人类体内,双酚类物质会代谢为葡萄糖醛酸和硫酸盐缀合物。最近的研究表明,硫酸盐缀合是最脆弱的人类(如生长中的胎儿)中双酚类物质代谢的重要途径。我们的目的是评估生物样本中常见双酚类物质的硫酸化动力学:双酚 A(BPA)、双酚 S(BPS)和双酚 F(BPF)。此外,我们还评估了这些双酚硫酸盐的雌激素激动剂效力和长期稳定性。BPS 和 BPF 硫酸盐通过化学合成制备。选择的双酚类物质的硫酸化动力学在人肝胞质液中进行测试,作为可溶性相 II 酶(包括肝磺基转移酶)的来源,通过 LC-MS/MS 进行定量。使用使用 hERα-Hela 9903 细胞系的验证转激活测定来确定雌激素激动剂效力。此外,还在各种条件下和储存期间检查了 BPA、BPS 和 BPF 硫酸盐的稳定性。BPA 和 BPS 的体外硫酸化遵循米氏动力学;BPF 的硫酸化遵循底物抑制模型。尽管这些双酚类物质的 K 值表明亲和力存在较大差异,但它们的硫酸化速率相当。BPA 和 BPS 硫酸盐不是 hERα 激动剂。在这些测试的介质条件下,双酚硫酸盐至少可以稳定 2 天。这些数据表明,双酚类物质的硫酸化是其生物转化的重要途径。与葡萄糖醛酸化相比,这些双酚类物质的硫酸化速率较慢,但 K 值相似。BPA 和 BPS 通过硫酸化进行代谢生物转化提供了它们的解毒作用,因为它们没有雌激素活性。

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