Moldable Plastics (Polycaprolactone) can be Acutely Toxic to Developing Zebrafish and Activate Nuclear Receptors in Mammalian Cells.

IF 5.4 2区 医学 Q2 MATERIALS SCIENCE, BIOMATERIALS ACS Biomaterials Science & Engineering Pub Date : 2024-07-09 DOI:10.1021/acsbiomaterials.4c00693
Bryan D James, Alexander V Medvedev, Sergei S Makarov, Robert K Nelson, Christopher M Reddy, Mark E Hahn
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Abstract

Popularized on social media, hand-moldable plastics are formed by consumers into tools, trinkets, and dental prosthetics. Despite the anticipated dermal and oral contact, manufacturers share little information with consumers about these materials, which are typically sold as microplastic-sized resin pellets. Inherent to their function, moldable plastics pose a risk of dermal and oral exposure to unknown leachable substances. We analyzed 12 moldable plastics advertised for modeling and dental applications and determined them to be polycaprolactone (PCL) or thermoplastic polyurethane (TPU). The bioactivities of the most popular brands advertised for modeling applications of each type of polymer were evaluated using a zebrafish embryo bioassay. While water-borne exposure to the TPU pellets did not affect the targeted developmental end points at any concentration tested, the PCL pellets were acutely toxic above 1 pellet/mL. The aqueous leachates of the PCL pellets demonstrated similar toxicity. Methanolic extracts from the PCL pellets were assayed for their bioactivity using the Attagene FACTORIAL platform. Of the 69 measured end points, the extracts activated nuclear receptors and transcription factors for xenobiotic metabolism (pregnane X receptor, PXR), lipid metabolism (peroxisome proliferator-activated receptor γ, PPARγ), and oxidative stress (nuclear factor erythroid 2-related factor 2, NRF2). By nontargeted high-resolution comprehensive two-dimensional gas chromatography (GC × GC-HRT), we tentatively identified several compounds in the methanolic extracts, including PCL oligomers, a phenolic antioxidant, and residues of suspected antihydrolysis and cross-linking additives. In a follow-up zebrafish embryo bioassay, because of its stated high purity, biomedical grade PCL was tested to mitigate any confounding effects due to chemical additives in the PCL pellets; it elicited comparable acute toxicity. From these orthogonal and complementary experiments, we suggest that the toxicity was due to oligomers and nanoplastics released from the PCL rather than chemical additives. These results challenge the perceived and assumed inertness of plastics and highlight their multiple sources of toxicity.

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可模塑塑料(聚己内酯)会对发育中的斑马鱼产生急性毒性,并激活哺乳动物细胞中的核受体。
可手模塑料在社交媒体上大受欢迎,消费者将其制成工具、小饰品和牙齿修复体。尽管预计会有皮肤和口腔接触,但制造商却很少与消费者分享有关这些材料的信息,它们通常以微型塑料大小的树脂颗粒形式出售。由于其固有的功能,可塑塑料会带来皮肤和口腔接触未知可浸出物质的风险。我们分析了 12 种用于建模和牙科应用的可塑塑料,并确定它们是聚己内酯(PCL)或热塑性聚氨酯(TPU)。使用斑马鱼胚胎生物测定法评估了每种聚合物中最受欢迎的建模应用品牌的生物活性。在任何测试浓度下,经水接触热塑性聚氨酯颗粒都不会影响目标发育终点,而 PCL 颗粒的急性毒性超过 1 颗粒/毫升。聚苯乙烯颗粒的水浸出物也显示出类似的毒性。使用 Attagene FACTORIAL 平台对 PCL 颗粒的甲醇提取物进行了生物活性检测。在 69 个测量终点中,萃取物激活了核受体和转录因子,用于异生物代谢(孕烷 X 受体,PXR)、脂质代谢(过氧化物酶体增殖激活受体 γ,PPARγ)和氧化应激(核因子红细胞 2 相关因子 2,NRF2)。通过非靶向高分辨率综合二维气相色谱法(GC × GC-HRT),我们初步确定了甲醇提取物中的几种化合物,包括 PCL 低聚物、一种酚类抗氧化剂以及疑似抗水解和交联添加剂的残留物。在后续的斑马鱼胚胎生物测定中,由于生物医用级聚氯乙烯的纯度较高,因此对其进行了测试,以减少聚氯乙烯颗粒中的化学添加剂造成的任何干扰效应;生物医用级聚氯乙烯的急性毒性与之相当。通过这些正交和互补实验,我们认为毒性是由 PCL 中释放的低聚物和纳米塑料而非化学添加剂引起的。这些结果对人们认为和假定的塑料惰性提出了挑战,并强调了塑料的多种毒性来源。
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来源期刊
ACS Biomaterials Science & Engineering
ACS Biomaterials Science & Engineering Materials Science-Biomaterials
CiteScore
10.30
自引率
3.40%
发文量
413
期刊介绍: ACS Biomaterials Science & Engineering is the leading journal in the field of biomaterials, serving as an international forum for publishing cutting-edge research and innovative ideas on a broad range of topics: Applications and Health – implantable tissues and devices, prosthesis, health risks, toxicology Bio-interactions and Bio-compatibility – material-biology interactions, chemical/morphological/structural communication, mechanobiology, signaling and biological responses, immuno-engineering, calcification, coatings, corrosion and degradation of biomaterials and devices, biophysical regulation of cell functions Characterization, Synthesis, and Modification – new biomaterials, bioinspired and biomimetic approaches to biomaterials, exploiting structural hierarchy and architectural control, combinatorial strategies for biomaterials discovery, genetic biomaterials design, synthetic biology, new composite systems, bionics, polymer synthesis Controlled Release and Delivery Systems – biomaterial-based drug and gene delivery, bio-responsive delivery of regulatory molecules, pharmaceutical engineering Healthcare Advances – clinical translation, regulatory issues, patient safety, emerging trends Imaging and Diagnostics – imaging agents and probes, theranostics, biosensors, monitoring Manufacturing and Technology – 3D printing, inks, organ-on-a-chip, bioreactor/perfusion systems, microdevices, BioMEMS, optics and electronics interfaces with biomaterials, systems integration Modeling and Informatics Tools – scaling methods to guide biomaterial design, predictive algorithms for structure-function, biomechanics, integrating bioinformatics with biomaterials discovery, metabolomics in the context of biomaterials Tissue Engineering and Regenerative Medicine – basic and applied studies, cell therapies, scaffolds, vascularization, bioartificial organs, transplantation and functionality, cellular agriculture
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