Predicting in vivo concentrations of dietary hop phytoestrogens by physiologically based kinetic modeling

Maja Stevanoska, Karsten Beekmann, Ans Punt, Shana Sturla, Georg Aichinger
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Abstract

Hop extracts containing prenylated polyphenols such as 8-prenylnaringenin (8-PN) and its precursor isoxanthohumol (iXN) are popular among women seeking natural alternatives to hormone therapy for postmenopausal symptoms. Due to structural similarities with estrogens, these compounds act as estrogen receptor agonists. Especially 8-PN, described as the most potent phytoestrogen known to date, poses a potential risk for endocrine disruption. Therefore, its use as a hormone replacement raises concerns for human health. However, a significant challenge in assessing the potential endocrine-disruptive effects of hop polyphenols is the lack of data on their toxicokinetics. Particularly, information on in vivo concentrations in target tissues is lacking. To address this gap, we developed a physiologically based kinetic (PBK) model tailored to female physiology. The model was used to predict the levels of hop polyphenols in human blood and target tissues under realistic exposure scenarios. The predictions suggest that iXN and 8-PN concentrations in target tissues reach the low nanomolar range after dietary supplementation. This study enhances our understanding of the safety profile of hop polyphenols and highlights the need for further research into their use as an alternative to hormone therapy in menopausal women.
通过基于生理学的动力学模型预测膳食中啤酒花植物雌激素的体内浓度
含有前炔多酚(如 8-前炔基柚皮素(8-PN)及其前体异黄腐醇(iXN))的啤酒花提取物在寻求激素疗法天然替代品以治疗绝经后症状的女性中很受欢迎。由于在结构上与雌激素相似,这些化合物可作为雌激素受体激动剂发挥作用。特别是 8-PN,它被称为迄今为止已知的最强效的植物雌激素,具有扰乱内分泌的潜在风险。因此,将其用作激素替代品会引发对人类健康的担忧。然而,在评估酒花多酚的潜在内分泌干扰作用时,一个重大的挑战是缺乏有关其毒物动力学的数据。特别是缺乏有关目标组织体内浓度的信息。为了填补这一空白,我们开发了一个针对女性生理特点的生理动力学(PBK)模型。该模型用于预测在实际暴露情况下啤酒花多酚在人体血液和靶组织中的含量。预测结果表明,膳食补充后,目标组织中的 iXN 和 8-PN 浓度会达到纳摩尔级的低水平。这项研究加深了我们对啤酒花多酚安全性的了解,并强调了进一步研究啤酒花多酚在更年期妇女中用作激素疗法替代品的必要性。
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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