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本文引用的文献

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Toxicity determinants of multi-walled carbon nanotubes: The relationship between functionalization and agglomeration.多壁碳纳米管的毒性决定因素:功能化与团聚之间的关系。
Toxicol Rep. 2016 Jan 19;3:230-243. doi: 10.1016/j.toxrep.2016.01.011. eCollection 2016.
2
The impact of subcellular location on the near infrared-mediated thermal ablation of cells by targeted carbon nanotubes.细胞内定位对靶向碳纳米管介导的近红外光热消融细胞的影响。
Nanotechnology. 2016 Oct 21;27(42):425102. doi: 10.1088/0957-4484/27/42/425102. Epub 2016 Sep 15.
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Bioaccumulation of Multiwall Carbon Nanotubes in Tetrahymena thermophila by Direct Feeding or Trophic Transfer.多壁碳纳米管通过直接投喂或营养转移在嗜热四膜虫中的生物累积
Environ Sci Technol. 2016 Aug 16;50(16):8876-85. doi: 10.1021/acs.est.6b01916. Epub 2016 Jul 26.
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Anthropogenic Carbon Nanotubes Found in the Airways of Parisian Children.巴黎儿童气道中发现的人为碳纳米管。
EBioMedicine. 2015 Oct 9;2(11):1697-704. doi: 10.1016/j.ebiom.2015.10.012. eCollection 2015 Nov.
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Toxicity assessment and bioaccumulation in zebrafish embryos exposed to carbon nanotubes suspended in Pluronic® F-108.暴露于悬浮在普朗尼克® F - 108中的碳纳米管的斑马鱼胚胎的毒性评估和生物累积
Nanotoxicology. 2016 Aug;10(6):689-98. doi: 10.3109/17435390.2015.1107147. Epub 2015 Nov 11.
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Scavenger receptor structure and function in health and disease.清道夫受体在健康与疾病中的结构和功能
Cells. 2015 May 22;4(2):178-201. doi: 10.3390/cells4020178.
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Adsorption of lactate dehydrogenase enzyme on carbon nanotubes: how to get accurate results for the cytotoxicity of these nanomaterials.乳酸脱氢酶在碳纳米管上的吸附:如何获得这些纳米材料细胞毒性的准确结果。
Langmuir. 2015 Mar 31;31(12):3635-43. doi: 10.1021/acs.langmuir.5b00631. Epub 2015 Mar 20.
8
Reprogramming cellular signaling machinery using surface-modified carbon nanotubes.
Chem Res Toxicol. 2015 Mar 16;28(3):296-305. doi: 10.1021/tx500480d. Epub 2015 Jan 14.
9
The importance of an extensive elemental analysis of single-walled carbon nanotube soot.单壁碳纳米管烟灰进行广泛元素分析的重要性。
Carbon N Y. 2014 Oct 1;77:912-919. doi: 10.1016/j.carbon.2014.06.005.
10
Lung macrophages "digest" carbon nanotubes using a superoxide/peroxynitrite oxidative pathway.肺巨噬细胞通过超氧化物/过氧亚硝酸盐氧化途径“消化”碳纳米管。
ACS Nano. 2014 Jun 24;8(6):5610-21. doi: 10.1021/nn406484b. Epub 2014 Jun 4.

细胞相关碳纳米管的定量分析:巨噬细胞对羧化碳纳米管的选择性结合和积累。

Quantitation of cell-associated carbon nanotubes: selective binding and accumulation of carboxylated carbon nanotubes by macrophages.

机构信息

a Department of Biological Sciences , The University of Texas at Dallas , Richardson , TX , USA.

b Department of Chemistry and Biochemistry , The University of Texas at Dallas , Richardson , TX , USA.

出版信息

Nanotoxicology. 2018 Sep;12(7):677-698. doi: 10.1080/17435390.2018.1472309. Epub 2018 May 26.

DOI:10.1080/17435390.2018.1472309
PMID:29804493
原文链接:https://pmc.ncbi.nlm.nih.gov/articles/PMC6209100/
Abstract

To understand the influence of carboxylation on the interaction of carbon nanotubes with cells, the amount of pristine multi-walled carbon nanotubes (P-MWNTs) or carboxylated multi-walled carbon nanotubes (C-MWNTs) coated with Pluronic F-108 that were accumulated by macrophages was measured by quantifying CNTs extracted from cells. Mouse RAW 264.7 macrophages and differentiated human THP-1 (dTHP-1) macrophages accumulated 80-100 times more C-MWNTs than P-MWNTs during a 24-h exposure at 37 °C. The accumulation of C-MWNTs by RAW 264.7 cells was not lethal; however, phagocytosis was impaired as subsequent uptake of polystyrene beads was reduced after a 20-h exposure to C-MWNTs. The selective accumulation of C-MWNTs suggested that there might be receptors on macrophages that bind C-MWNTs. The binding of C-MWNTs to macrophages was measured as a function of concentration at 4 °C in the absence of serum to minimize the potential interference by serum proteins or temperature-dependent uptake processes. The result was that the cells bound 8.7 times more C-MWNTs than P-MWNTs, consistent with the selective accumulation of C-MWNTs at 37 °C. In addition, serum strongly antagonized the binding of C-MWTS to macrophages, suggesting that serum contained inhibitors of binding. Moreover, inhibitors of class A scavenger receptor (SR-As) reduced the binding of C-MWNTs by about 50%, suggesting that SR-As contribute to the binding and endocytosis of C-MWNTs in macrophages but that other receptors may also be involved. Altogether, the evidence supports the hypothesis that macrophages contain binding sites selective for C-MWNTs that facilitate the high accumulation of C-MWNTs compared to P-MWNTs.

摘要

为了理解羧化作用对碳纳米管与细胞相互作用的影响,通过定量提取自细胞的 CNTs 来测量被巨噬细胞积累的未功能化多壁碳纳米管 (P-MWNTs) 或羧化多壁碳纳米管 (C-MWNTs) 上包裹的普朗尼克 F-108 的量。在 37°C 下暴露 24 小时,RAW 264.7 巨噬细胞和分化的人 THP-1(dTHP-1)巨噬细胞积累的 C-MWNTs 比 P-MWNTs 多 80-100 倍。RAW 264.7 细胞对 C-MWNTs 的积累并不致命;然而,吞噬作用受损,因为在暴露于 C-MWNTs 20 小时后,聚苯乙烯珠的后续摄取减少。C-MWNTs 的选择性积累表明巨噬细胞上可能存在与 C-MWNTs 结合的受体。在不存在血清的情况下,在 4°C 下作为浓度的函数测量 C-MWNTs 与巨噬细胞的结合,以最大程度地减少血清蛋白或温度依赖性摄取过程的潜在干扰。结果是细胞与 C-MWNTs 的结合是 P-MWNTs 的 8.7 倍,这与 37°C 时 C-MWNTs 的选择性积累一致。此外,血清强烈拮抗 C-MWTS 与巨噬细胞的结合,表明血清中含有结合抑制剂。此外,A 类清道夫受体 (SR-As) 的抑制剂使 C-MWNTs 的结合减少了约 50%,表明 SR-As 有助于巨噬细胞中 C-MWNTs 的结合和内吞作用,但也可能涉及其他受体。总之,证据支持这样一种假设,即巨噬细胞含有对 C-MWNTs 具有选择性的结合位点,这有助于与 P-MWNTs 相比,C-MWNTs 的高积累。