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关于测量纳米颗粒尺寸的操作方面

On the Operational Aspects of Measuring Nanoparticle Sizes.

作者信息

Teulon Jean-Marie, Godon Christian, Chantalat Louis, Moriscot Christine, Cambedouzou Julien, Odorico Michael, Ravaux Johann, Podor Renaud, Gerdil Adèle, Habert Aurélie, Herlin-Boime Nathalie, Chen Shu-Wen W, Pellequer Jean-Luc

机构信息

Univ. Grenoble Alpes, CEA, CNRS, IBS, F-38000 Grenoble, France.

CEA, iBEB, LIRM, F-30207 Bagnols sur Cèze, France.

出版信息

Nanomaterials (Basel). 2018 Dec 23;9(1):18. doi: 10.3390/nano9010018.

Abstract

Nanoparticles are defined as elementary particles with a size between 1 and 100 nm for at least 50% (in number). They can be made from natural materials, or manufactured. Due to their small sizes, novel toxicological issues are raised and thus determining the accurate size of these nanoparticles is a major challenge. In this study, we performed an intercomparison experiment with the goal to measure sizes of several nanoparticles, in a first step, calibrated beads and monodispersed SiO₂ Ludox®, and, in a second step, nanoparticles (NPs) of toxicological interest, such as Silver NM-300 K and PVP-coated Ag NPs, Titanium dioxide A12, P25(Degussa), and E171(A), using commonly available laboratory techniques such as transmission electron microscopy, scanning electron microscopy, small-angle X-ray scattering, dynamic light scattering, wet scanning transmission electron microscopy (and its dry state, STEM) and atomic force microscopy. With monomodal distributed NPs (polystyrene beads and SiO₂ Ludox®), all tested techniques provide a global size value amplitude within 25% from each other, whereas on multimodal distributed NPs (Ag and TiO₂) the inter-technique variation in size values reaches 300%. Our results highlight several pitfalls of NP size measurements such as operational aspects, which are unexpected consequences in the choice of experimental protocols. It reinforces the idea that averaging the NP size from different biophysical techniques (and experimental protocols) is more robust than focusing on repetitions of a single technique. Besides, when characterizing a heterogeneous NP in size, a size distribution is more informative than a simple average value. This work emphasizes the need for nanotoxicologists (and regulatory agencies) to test a large panel of different techniques before making a choice for the most appropriate technique(s)/protocol(s) to characterize a peculiar NP.

摘要

纳米颗粒被定义为至少50%(按数量计)尺寸在1至100纳米之间的基本颗粒。它们可以由天然材料制成,也可以是人工制造的。由于其尺寸小,引发了新的毒理学问题,因此确定这些纳米颗粒的准确尺寸是一项重大挑战。在本研究中,我们进行了一项比对实验,目的是测量几种纳米颗粒的尺寸。第一步,使用校准珠和单分散的SiO₂ 氯丁橡胶,第二步,使用透射电子显微镜、扫描电子显微镜、小角X射线散射、动态光散射、湿扫描透射电子显微镜(及其干燥状态,扫描透射电子显微镜)和原子力显微镜等常用实验室技术,测量具有毒理学意义的纳米颗粒(NP),如银NM - 300 K和聚乙烯吡咯烷酮包覆的银纳米颗粒、二氧化钛A12、P25(德固赛)和E171(A)。对于单峰分布的纳米颗粒(聚苯乙烯珠和SiO₂ 氯丁橡胶),所有测试技术提供的整体尺寸值幅度相互之间相差在25%以内,而对于多峰分布的纳米颗粒(银和二氧化钛),尺寸值的技术间差异达到300%。我们的结果突出了纳米颗粒尺寸测量的几个陷阱,如操作方面,这是实验方案选择中意想不到的后果。这强化了这样一种观点,即从不同生物物理技术(和实验方案)获取的纳米颗粒尺寸平均值比专注于单一技术的重复测量更可靠。此外,在表征尺寸不均一的纳米颗粒时,尺寸分布比简单的平均值更具信息量。这项工作强调了纳米毒理学家(和监管机构)在选择最合适的技术/方案来表征特定纳米颗粒之前,需要测试大量不同技术的必要性。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/c52c/6359205/96140869990a/nanomaterials-09-00018-g001.jpg

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