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基于独立专家组的研究结果:评估全氟辛酸(PFOA)和全氟辛烷磺酸(PFOS)的化学诱导免疫毒性的证据权重。

Weight of evidence evaluation for chemical-induced immunotoxicity for PFOA and PFOS: findings from an independent panel of experts.

机构信息

GSI Environmental, Houston, TX, USA.

GSI Environmental, Austin, TX, USA.

出版信息

Crit Rev Toxicol. 2023 Jan;53(1):34-51. doi: 10.1080/10408444.2023.2194913. Epub 2023 Apr 28.

Abstract

Immunotoxicity is the critical endpoint used by some regulatory agencies to establish toxicity values for perfluorooctanoic acid (PFOA) and perfluorooctane sulfonate (PFOS). However, the hypothesis that exposure to certain per- and polyfluoroalkyl substances (PFAS) causes immune dysregulation is subject to much debate. An independent, international expert panel was engaged utilizing methods to reduce bias and "groupthink". The panel concluded there is moderate evidence that PFOS and PFOA are immunotoxic, based primarily on evidence from animal data. However, species concordance and human relevance cannot be well established due to data limitations. The panel recommended additional testing that includes longer-term exposures, evaluates both genders, includes other species of animals, tests lower dose levels, assesses more complete measures of immune responses, and elucidates the mechanism of action. Panel members agreed that the Faroe Islands cohort data should not be used as the primary basis for deriving PFAS risk assessment values. The panel agreed that vaccine antibody titer is not useful as a stand-alone metric for risk assessment. Instead, PFOA and PFOS toxicity values should rely on multiple high-quality studies, which are currently not available for immune suppression. The panel concluded that the available PFAS immune epidemiology studies suffer from weaknesses in study design that preclude their use, whereas available animal toxicity studies provide comprehensive dataset to derive points of departure (PODs) for non-immune endpoints. The panel recommends accounting for potential PFAS immunotoxicity by applying a database uncertainty factor to POD values derived from animal studies for other more robustly supported critical effects.

摘要

免疫毒性是一些监管机构用来确定全氟辛酸(PFOA)和全氟辛烷磺酸(PFOS)毒性值的关键终点。然而,接触某些全氟和多氟烷基物质(PFAS)会导致免疫失调的假设存在很大争议。利用减少偏见和“群体思维”的方法,成立了一个独立的国际专家小组。该小组得出结论,有中度证据表明 PFOS 和 PFOA 具有免疫毒性,主要基于动物数据的证据。然而,由于数据限制,无法很好地确定物种一致性和人类相关性。小组建议进行额外的测试,包括长期暴露、评估两性、包括其他动物物种、测试较低的剂量水平、评估更完整的免疫反应措施,并阐明作用机制。小组成员一致认为,法罗群岛队列数据不应作为制定 PFAS 风险评估值的主要依据。小组成员一致认为,疫苗抗体滴度不能作为风险评估的独立指标。相反,PFOA 和 PFOS 的毒性值应依赖于多个高质量的研究,而目前这些研究还没有用于免疫抑制。小组得出结论,现有 PFAS 免疫流行病学研究在研究设计上存在缺陷,因此无法使用,而现有的动物毒性研究提供了全面的数据集,可以为其他更有力支持的关键效应推导出起始点(POD)。小组建议通过对动物研究中推导出的非免疫终点的起始点值应用数据库不确定系数,来考虑潜在的 PFAS 免疫毒性。

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