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Releases from transparent blue automobile coatings containing nanoscale copper phthalocyanine and their effects on J774 A1 macrophages

机译:含有纳米级酞菁铜的透明蓝色汽车涂料的释放及其对J774 A1巨噬细胞的影响

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摘要

Nanoscale copper phthalocyanine (n-CuPc) is a pigment widely used in paints to enhance automobile coatings and to make colors transparent and more appealing to users. Despite the benefits, n-CuPc can potentially be released into the environment and pose risks in occupational settings. Assessing the toxicity of released n-CuPc-containing fragments is thus important for the acceptance of n-CuPc products. This paper presents the first combined study addressing both the release of n-CuPc-containing fragments from commercial coatings in realistic occupational situations and the hazard of the released fragments using a macrophage model. Sanding was used to produce fragments from automobile coatings with n-CuPc as well as from a reference coating with the same matrix composition but without n-CuPc. Size distribution and agglomeration of these fragments in Rosewell Park Memorial Institute (RPMI) cell culture medium was studied before conducting a battery of cytotoxicity experiments. Cell viability and reactive oxygen species (ROS) production were conducted and particle localization within cells was analyzed. The results show similar size and number distribution of fragments when comparing the reference and n-CuPc fragments. The n-CuPc fragments showed higher agglomeration in RPMI than pristine n-CuPc. We found that toxicity of the n-CuPc fragments and reference materials was similar (EC50 Frag n-CuPc = 242.9 μg mlâ\u88\u92 1; EC50 Frag Refer = 241.6 μg mlâ\u88\u921) and below the toxicity of pristine n-CuPc (EC50 n-CuPc = 151.1 μg mlâ\u88\u921). The results demonstrated that embedding n-CuPc in matrix used in automobile coatings reduced the toxicity and release when n-CuPc is used in paints. Our finding can be used to support design of n-CuPc-enabled products used in automobile applications.
机译:纳米级酞菁铜(n-CuPc)是广泛用于涂料中的颜料,可增强汽车涂料并使其颜色透明并吸引用户。尽管有这些好处,n-CuPc仍可能释放到环境中,并在职业环境中带来风险。因此,评估释放的含n-CuPc片段的毒性对于n-CuPc产品的接受很重要。本文提出了第一个联合研究,既解决了在实际职业环境中从商用涂料中释放出含n-CuPc的碎片,又使用巨噬细胞模型探讨了释放的碎片的危害。使用打磨从含有n-CuPc的汽车涂料以及具有相同基质组成但不含n-CuPc的参考涂料中产生碎片。在进行一系列细胞毒性实验之前,研究了这些片段在Rosewell Park Memorial Institute(RPMI)细胞培养基中的大小分布和聚集。进行细胞活力和活性氧(ROS)产生,并分析细胞内的颗粒定位。比较参考片段和n-CuPc片段时,结果显示出相似的片段大小和数量分布。 n-CuPc片段在RPMI中显示出比原始n-CuPc更高的团聚。我们发现,n-CuPc片段和参考材料的毒性相似(EC50 Frag n-CuPc = 242.9μgmlâu88\ u92 1; EC50 Frag Refer = 241.6μgmlâu88\ u921),且低于原始n的毒性-CuPc(EC50 n-CuPc = 151.1微克ml \ u88 \ u921)。结果表明,将n-CuPc嵌入汽车涂料中可降低n-CuPc在涂料中的毒性和释放。我们的发现可用于支持汽车应用中支持n-CuPc的产品的设计。

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