Use of in vitro ADME methods to identify suitable analogs of homosalate and octisalate for use in a read‐across safety assessment

广告 化学 生物利用度 水杨酸 体外 关键质量属性 药理学 体外毒理学 生物化学 组合化学 生物 物理化学 粒径
作者
Sébastien Grégoire,Anne Moustié,Guillaume Léreaux,L. Roussel,Nicola J. Hewitt
出处
期刊:Journal of Applied Toxicology [Wiley]
卷期号:44 (7): 1067-1083 被引量:2
标识
DOI:10.1002/jat.4603
摘要

Abstract Case studies are needed to demonstrate the use of human‐relevant New Approach Methodologies in cosmetics ingredient safety assessments. For read‐across assessments, it is crucial to compare the target chemical with the most appropriate analog; therefore, reliable analog selection should consider physicochemical properties, bioavailability, metabolism, as well as the bioactivity of potential analogs. To complement in vitro bioactivity assays, we evaluated the suitability of three potential analogs for the UV filters, homosalate and octisalate, according to their in vitro ADME properties. We describe how technical aspects of conducting assays for these highly lipophilic chemicals were addressed and interpreted. There were several properties that were common to all five chemicals: they all had similar stability in gastrointestinal fluids (in which no hydrolysis to salicylic occurred); were not substrates of the P‐glycoprotein efflux transporter; were highly protein bound; and were hydrolyzed to salicylic acid (which was also a major metabolite). The main properties differentiating the chemicals were their permeability in Caco‐2 cells, plasma stability, clearance in hepatic models, and the extent of hydrolysis to salicylic acid. Cyclohexyl salicylate, octisalate, and homosalate were identified suitable analogs for each other, whereas butyloctyl salicylate exhibited ADME properties that were markedly different, indicating it is unsuitable. Isoamyl salicylate can be a suitable analog with interpretation for octisalate. In conclusion, in vitro ADME properties of five chemicals were measured and used to pair target and potential analogs. This study demonstrates the importance of robust ADME data for the selection of analogs in a read‐across safety assessment.
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