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聚合物的化学稳定作用:对皮肤接触添加剂的影响

Chemical stabilization of polymers: Implications for dermal exposure to additives.

作者信息

Bartsch N, Girard M, Schneider L, Weijgert V Van De, Wilde A, Kappenstein O, Vieth B, Hutzler C, Luch A

机构信息

a Department of Chemical and Product Safety , German Federal Institute for Risk Assessment (BfR) , Berlin , Germany.

出版信息

J Environ Sci Health A Tox Hazard Subst Environ Eng. 2018 Apr 16;53(5):405-420. doi: 10.1080/10934529.2017.1412192. Epub 2018 Jan 15.

Abstract

Technical benefits of additives in polymers stand in marked contrast to their associated health risks. Here, a multi-analyte method based on gas chromatography coupled to tandem mass spectrometry (GC-MS/MS) was developed to quantify polymer additives in complex matrices such as low-density polyethylene (LDPE) and isolated human skin layers after dermal exposure ex vivo. That way both technical aspects and dermal exposure were investigated. The effects of polymer additivation on the material were studied using the example of LDPE. To this end, a tailor-made polymer was applied in aging studies that had been furnished with two different mixtures of phenol- and diarylamine-based antioxidants, plasticizers and processing aids. Upon accelerated thermo-oxidative aging of the material, the formation of LDPE degradation products was monitored with attenuated total reflectance-Fourier transformed infrared (ATR-FTIR) spectroscopy. Compared to pure LDPE, a protective effect of added antioxidants could be observed on the integrity of the polymer. Further, thermo-oxidative degradation of the additives and its kinetics were investigated using LDPE or squalane as matrix. The half-lives of additives in both matrices revealed significant differences between the tested additives as well as between LDPE and squalane. For instance, 2-tert-butyl-6-[(3-tert-butyl-2-hydroxy-5-methylphenyl)methyl]-4-methylphenol (Antioxidant 2246) showed a half-life 12 times lower when incorporated in LDPE as compared to squalane. As a model for dermal exposure of consumers, human skin was brought into contact with the tailor-made LDPE containing additives ex vivo in static Franz diffusion cells. The skin was then analyzed for additives and decomposition products. This study proved 10 polymer additives of diverse pysicochemical properties and functionalities to migrate out of the polymer and eventually overcome the intact human skin barrier during contact. Moreover, their individual distribution within distinct skin layers was demonstrated. This is exemplified by the penetration of the procarcinogenic antioxidant N-phenylnaphthalen-2-amine (Neozon D) into the viable epidermis and the permeation through the skin of the neurotoxic plasticizer N-butylbenzenesulfonamide (NBBS). In addition, the analyses of additive degradation products in the isolated skin layers revealed the presence of 2-tert-butyl-4-methylphenol in all layers after contact to a polymer with substances of origin like Antioxidant 2246. Thus, attention needs to be paid to absorption of polymer additives together with their degradation products when it comes to dermal exposure assessment.

摘要

聚合物中添加剂的技术优势与其相关的健康风险形成了鲜明对比。在此,开发了一种基于气相色谱-串联质谱联用(GC-MS/MS)的多分析物方法,用于定量复杂基质中的聚合物添加剂,如低密度聚乙烯(LDPE)以及离体皮肤暴露后分离出的人体皮肤层中的添加剂。通过这种方式,对技术层面和皮肤暴露情况都进行了研究。以LDPE为例,研究了聚合物添加对材料的影响。为此,在老化研究中应用了一种特制的聚合物,该聚合物含有两种不同的基于苯酚和二芳基胺的抗氧化剂、增塑剂和加工助剂的混合物。在对材料进行加速热氧化老化时,用衰减全反射-傅里叶变换红外光谱(ATR-FTIR)监测LDPE降解产物的形成。与纯LDPE相比,可以观察到添加的抗氧化剂对聚合物完整性具有保护作用。此外,以LDPE或角鲨烷为基质,研究了添加剂的热氧化降解及其动力学。两种基质中添加剂的半衰期显示,所测试的添加剂之间以及LDPE和角鲨烷之间存在显著差异。例如,2-叔丁基-6-[(3-叔丁基-2-羟基-5-甲基苯基)甲基]-4-甲基苯酚(抗氧化剂2246)掺入LDPE时的半衰期比掺入角鲨烷时低12倍。作为消费者皮肤暴露的模型,将人体皮肤在静态Franz扩散池中与含有添加剂的特制LDPE离体接触。然后对皮肤中的添加剂和分解产物进行分析。该研究证明,10种具有不同物理化学性质和功能的聚合物添加剂会从聚合物中迁移出来,并最终在接触过程中突破完整的人体皮肤屏障。此外,还展示了它们在不同皮肤层中的各自分布情况。致癌前体抗氧化剂N-苯基萘-2-胺(Neozon D)渗透到活表皮以及神经毒性增塑剂N-丁基苯磺酰胺(NBBS)透过皮肤就是例证。此外,对分离出的皮肤层中添加剂降解产物的分析表明,在与含有抗氧化剂2246等来源物质的聚合物接触后,所有皮肤层中都存在2-叔丁基-4-甲基苯酚。因此,在进行皮肤暴露评估时,需要关注聚合物添加剂及其降解产物的吸收情况。

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