Improved Dispersion Method of Multi-wall Carbon Nanotube for Inhalation Toxicity Studies of Experimental Animals

Overview

Journal J Toxicol Sci

Specialty Toxicology

Date 2013 Jul 5

PMID 23824017

Citations 15

Authors

Yuhji Taquahashi

Yukio Ogawa

Atsuya Takagi

Masaki Tsuji

Koichi Morita

Jun Kanno

Affiliations

Soon will be listed here.

Abstract

A multi-wall carbon nanotube (MWCNT) product Mitsui MWNT-7 is a mixture of dispersed single fibers and their agglomerates/aggregates. In rodents, installation of such mixture induces inflammatory lesions triggered predominantly by the aggregates/agglomerates at the level of terminal bronchiole of the lungs. In human, however, pulmonary toxicity induced by dispersed single fibers that reached the lung alveoli is most important to assess. Therefore, a method to generate aerosol predominantly consisting of dispersed single fibers without changing their length and width is needed for inhalation studies. Here, we report a method (designated as Taquann method) to effectively remove the aggregate/agglomerates and enrich the well-dispersed singler fibers in dry state without dispersant and without changing the length and width distribution of the single fibers. This method is base on two major concept; liquid-phase fine filtration and critical point drying to avoid re-aggregation by surface tension. MWNT-7 was suspended in Tert-butyl alcohol, freeze-and-thawed, filtered by a vibrating 25 µm mesh Metallic Sieve, snap-frozen by liquid nitrogen, and vacuum-sublimated (an alternative method to carbon dioxide critical point drying). A newly designed direct injection system generated well-dispersed aerosol in an inhalation chamber. The lung of mice exposed to the aerosol contained single fibers with a length distribution similar to the original and the Taquann-treated sample. Taquann method utilizes inexpensive materials and equipments mostly found in common biological laboratories, and prepares dry powder ready to make well-dispersed aerosol. This method and the chamber with direct injection system would facilitate the inhalation toxicity studies more relevant to human exposure.

Citing Articles

Time-Course of Transcriptomic Change in the Lungs of F344 Rats Repeatedly Exposed to a Multiwalled Carbon Nanotube in a 2-Year Test.

Hojo M, Maeno A, Sakamoto Y, Yamamoto Y, Taquahashi Y, Hirose A Nanomaterials (Basel). 2023; 13(14).

PMID: 37513116 PMC: 10383707. DOI: 10.3390/nano13142105.

In vivo genotoxicity assessment of a multiwalled carbon nanotube in a mouse ex vivo culture.

Horibata K, Takasawa H, Hojo M, Taquahashi Y, Shigano M, Yokota S Genes Environ. 2022; 44(1):24.

PMID: 36258253 PMC: 9580184. DOI: 10.1186/s41021-022-00253-2.

Two-year intermittent exposure of a multiwalled carbon nanotube by intratracheal instillation induces lung tumors and pleural mesotheliomas in F344 rats.

Hojo M, Maeno A, Sakamoto Y, Ohnuki A, Tada Y, Yamamoto Y Part Fibre Toxicol. 2022; 19(1):38.

PMID: 35590372 PMC: 9118836. DOI: 10.1186/s12989-022-00478-7.

Spatiotemporal Small Non-coding RNAs Expressed in the Germline as an Early Biomarker of Testicular Toxicity and Transgenerational Effects Caused by Prenatal Exposure to Nanosized Particles.

Yokota S, Takeda K, Oshio S Front Toxicol. 2022; 3:691070.

PMID: 35295114 PMC: 8915876. DOI: 10.3389/ftox.2021.691070.

Histological sequence of the development of rat mesothelioma by MWCNT, with the involvement of apolipoproteins.

Hojo M, Yamamoto Y, Sakamoto Y, Maeno A, Ohnuki A, Suzuki J Cancer Sci. 2021; 112(6):2185-2198.

PMID: 33665882 PMC: 8177772. DOI: 10.1111/cas.14873.