Comparative inhalation toxicity of multi-wall carbon nanotubes, graphene, graphite nanoplatelets and low surface carbon black

Ma‐Hock, Lan; Strauss, Volker; Treumann, Silke; Küttler, Karin; Wohlleben, Wendel; Hofmann, Thomas; Gröters, Sibylle; Wiench, Karin; Ravenzwaay, Bennard van; Landsiedel, Robert

doi:10.1186/1743-8977-10-23

Cited by 169 publications

(130 citation statements)

References 48 publications

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“…For example, in vivo studies are often carried out with lower doses per lung surface (excluding overload experiments). For various carbonaceous materials, it has been demonstrated that at similar doses, carbon black and graphite have no effect (0.1 or 0.03 µg/cm 2 , respectively; an estimate of the rat lung surface area 0.3 m 2 was used in this calculation (Brown et al, 2005)), but graphene and multiwall carbon nanotubes do have an effect (0.03 or 0.01 µg/cm 2 , respectively (Ma-Hock et al, 2013)). Moreover, in vivo investigations have shown that both the dosing rate and the delivered dose are responsible for toxicological effects.…”

Section: Tab 3: System Specifications For the Mts Assay As Defined Bmentioning

confidence: 99%

Toward achieving harmonization in a nanocytotoxicity assay measurement through an interlaboratory comparison study

Elliott

Rösslein

Song

et al. 2017

ALTEX

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SummaryDevelopment of reliable cell-based nanotoxicology assays is important for evaluation of potentially hazardous engineered nanomaterials. Challenges to producing a reliable assay protocol include working with nanoparticle dispersions and living cell lines, and the potential for nano-related interference effects. Here we demonstrate the use of a 96-well plate design with several measurement controls and an interlaboratory comparison study involving five laboratories to characterize the robustness of a nanocytotoxicity MTS cell viability assay based on the A549 cell line. The consensus EC 50 values were 22.1 mg/L (95% confidence intervals 16.9 mg/L to 27.2 mg/L) and 52.6 mg/L (44.1 mg/L to 62.6 mg/L) for positively charged polystyrene nanoparticles for the serum-free and serum conditions, respectively, and 49.7 µmol/L (47.5 µmol/L to 51.5 µmol/L) and 77.0 µmol/L (54.3 µmol/L to 99.4 µmol/L) for positive chemical control cadmium sulfate for the serum-free and serum conditions, respectively. Results from the measurement controls can be used to evaluate the sources of variability and their relative magnitudes within and between laboratories. This information revealed steps of the protocol that may need to be modified to improve the overall robustness and precision. The results suggest that protocol details such as cell line ID, media exchange, cell handling, and nanoparticle dispersion are critical to ensure protocol robustness and comparability of nanocytotoxicity assay results. The combination of system control measurements and interlaboratory comparison data yielded insights that would not have been available by either approach by itself.

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Section: Tab 3: System Specifications For the Mts Assay As Defined Bmentioning

confidence: 99%

Toward achieving harmonization in a nanocytotoxicity assay measurement through an interlaboratory comparison study

Elliott

Rösslein

Song

et al. 2017

ALTEX

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“…Levels of statistical significance: *p 0.05 and **p 0.01 compared to appropriate control group. between the 'synthetic' and 'biological' identities of nanoparticle formulations and observed in vivo effects (Ma-Hock et al, 2013). Lastly, human exposure to nanoparticles rarely, if ever, occurs to well-defined nanoparticle preparations.…”

Section: Discussionmentioning

confidence: 99%

Route-dependent systemic and local immune effects following exposure to solutions prepared from titanium dioxide nanoparticles

Auttachoat

McLoughlin

White

et al. 2013

Journal of Immunotoxicology

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Nanoparticle titanium dioxide (nano-TiO 2 ) is a white pigment widely used in foods, sunscreens, and other cosmetic products. However, it remains unclear whether exposure to nano-TiO 2 results in immunosuppressive effects or induces a contact hypersensitivity response. To address these data gaps, studies were conducted with the hypothesis that nano-TiO 2 exposure could alter immune responses. After 28 days of oral gavage, nano-TiO 2 (1.25-250 mg/kg in 0.5% methylcellulose) produced no significant effects on innate, humoral, or cell-mediated immune functions in female B6C3F1 mice. Furthermore, there were no effects on the weights of selected organs (spleen, thymus, liver, lung, and kidneys with adrenals). Following dermal exposure on the ears for 3 days, nano-TiO 2 (2.5-10% w/v in 4:1 acetone:olive oil) did not affect auricular lymph node cell proliferation, although an irritancy response was observed following treatment with 5% and 10% nano-TiO 2 . Dermal sensitization (2.5-10%) on the back and subsequent challenge (10%) on the right ear with nano-TiO 2 produced no significant effects on percentage ear swelling in the Mouse Ear Swelling Test (MEST). However, when nano-TiO 2 was injected subcutaneously along the mid-line on top of the head at 125-250 mg/kg (in 0.5% methylcellulose), significant increases in auricular lymph node cell proliferation resulted. These results demonstrate that immune effects of nano-TiO 2 exposure are route-of-exposure dependent, and they suggest that irritancy and/or potential hypersensitivity responses may occur following parenteral exposure or dermal administration of nano-TiO 2 to compromised skin.

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“…The toxicity of MWCNTs is more adverse in the case of inhalation as compared to oral exposure. Rats exposed to 2.5 mg/m 3 MWCNTs for 6 h/day during 5 consecutive days using a head-nose system demonstrated signs of pulmonary toxicity such as, microgranulomas and diffuse alveolar histiocytosis (Ma-Hock et al, 2013). After a 13-week exposure period, the inhalation of 2.5 mg/m 3 MWCNTs induced systemic inflammation and histopathological abnormalities in the lungs, lymph nodes, nasal cavity, larynx, and trachea (Ma-Hock et al, 2009).…”

Section: Mammalian Toxicity (Rodents)mentioning

confidence: 99%

Nanomaterials in the Environment: Perspectives on in Vivo Terrestrial Toxicity Testing

Mendonça

Rizoli

Ávila

et al. 2017

Front. Environ. Sci.

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Over the last decade, engineered nanomaterials (NMs) brought a revolutionary development in many sectors of human life including electronics, paints, textiles, food, agriculture, and health care. However, the exponential growth in the number of NMs applications resulted in uncertainties regarding their environmental impacts. Currently, the common approach for assessing the toxicity of NMs such as, carbon-(fullerenes, single-and multi-walled carbon nanotubes), mineral-(gold and silver nanoparticles, cerium and zinc oxide, silicon and titanium dioxide), and organic-based NMs (dendrimers) includes standard guidelines applied to all chemical compounds. Nevertheless, NMs differ from traditional materials as their physicochemical and surface properties influence the toxic rather than their composition alone. Considering such NMs specificities, adaptations in some methods are necessary to ensure that environmental and human health risks are accurately investigated. In this context, the focus of this mini-review is to summarize the current knowledge in nanotoxicology regarding relevant organisms and experimental assays for assessing the terrestrial toxicity of NMs.

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Comparative inhalation toxicity of multi-wall carbon nanotubes, graphene, graphite nanoplatelets and low surface carbon black

Cited by 169 publications

References 48 publications

Toward achieving harmonization in a nanocytotoxicity assay measurement through an interlaboratory comparison study

Toward achieving harmonization in a nanocytotoxicity assay measurement through an interlaboratory comparison study

Route-dependent systemic and local immune effects following exposure to solutions prepared from titanium dioxide nanoparticles

Nanomaterials in the Environment: Perspectives on in Vivo Terrestrial Toxicity Testing

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