Toxicity assessment of zinc oxide nanoparticles using sub-acute and sub-chronic murine inhalation models

Adamcakova‐Dodd, Andrea; Stebounova, Larissa V.; Kim, Jong Sung; Vorrink, Sabine U.; Ault, Andrew P.; O’Shaughnessy, Patrick T.; Grassian, Vicki H.; Thorne, Peter S.

doi:10.1186/1743-8977-11-15

Cited by 205 publications

(119 citation statements)

References 49 publications

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“…Seiffert et al [27] conducted an intratracheal instillation test of silver nanoparticles, and the exposure induced a transient KC concentration in BALF, while the chemokine expression pattern was accompanied by neutrophil influx in the lung. An inhalation exposure of ZnO nanoparticles with low toxicity did not induce neutrophil influx or an increase the concentration of KC in BALF [28].…”

Section: Endpointsmentioning

confidence: 80%

Significance of Intratracheal Instillation Tests for the Screening of Pulmonary Toxicity of Nanomaterials

Morimoto

Izumi

Yoshiura

et al. 2017

J UOEH

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: Inhalation tests are the gold standard test for the estimation of the pulmonary toxicity of respirable materials. Intratracheal instillation tests have been used widely, but they yield limited evidence of the harmful effects of respirable materials. We reviewed the effectiveness of intratracheal instillation tests for estimating the hazards of nanomaterials, mainly using research papers featuring intratracheal instillation and inhalation tests centered on a Japanese national project. Compared to inhalation tests, intratracheal instillation tests induced more acute inflammatory responses in the animal lung due to a bolus effect regardless of the toxicity of the nanomaterials. However, nanomaterials with high toxicity induced persistent inflammation in the chronic phase, and nanomaterials with low toxicity induced only transient inflammation. Therefore, in order to estimate the harmful effects of a nanomaterial, an observation period of 3 months or 6 months following intratracheal instillation is necessary. Among the endpoints of pulmonary toxicity, cell count and percentage of neutrophil, chemokines for neutrophils and macrophages, and oxidative stress markers are considered most important. These markers show persistent and transient responses in the lung from nanomaterials with high and low toxicity, respectively. If the evaluation of the pulmonary toxicity of nanomaterials is performed in not only the acute but also the chronic phase in order to avoid the bolus effect of intratracheal instillation and inflammatory-related factors that are used as endpoints of pulmonary toxicity, we speculate that intratracheal instillation tests can be useful for screening for the identification of the hazard of nanomaterials through pulmonary inflammation.

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Section: Endpointsmentioning

confidence: 80%

Significance of Intratracheal Instillation Tests for the Screening of Pulmonary Toxicity of Nanomaterials

Morimoto

Izumi

Yoshiura

et al. 2017

J UOEH

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“…27 Studies reported that ZnO NPs cause no toxicity to human cells and only low subchronic toxicity to rodents. [28][29][30] Furthermore, a previous study using Drosophila had reported no toxicity observed upon the ingestion of ZnO NPs. 21 On the other hand, another earlier study assessing the genotoxicity and oxidative stress induced by ZnO NPs in Drosophila showed a weak genotoxicity of ZnO NPs.…”

Section: Introductionmentioning

confidence: 99%

Zinc oxide nanoparticles exhibit cytotoxicity and genotoxicity through oxidative stress responses in human lung fibroblasts and <em>Drosophila melanogaster</em>

Yong

Hande³

et al. 2017

IJN

198

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Background Although zinc oxide nanoparticles (ZnO NPs) have been widely used, there has been an increasing number of reports on the toxicity of ZnO NPs. However, study on the underlying mechanisms under in vivo conditions is insufficient. Methods In this study, we investigated the toxicological profiles of ZnO NPs in MRC5 human lung fibroblasts in vitro and in an in vivo model using the fruit fly Drosophila melanogaster . A comprehensive study was conducted to evaluate the uptake, cytotoxicity, reactive oxygen species (ROS) formation, gene expression profiling and genotoxicity induced by ZnO NPs. Results For in vitro toxicity, the results showed that there was a significant release of extracellular lactate dehydrogenase and decreased cell viability in ZnO NP-treated MRC5 lung cells, indicating cellular damage and cytotoxicity. Generation of ROS was observed to be related to significant expression of DNA Damage Inducible Transcript ( DDIT3 ) and endoplasmic reticulum (ER) to nucleus signaling 1 ( ERN1 ) genes, which are ER stress-related genes. Oxidative stress induced DNA damage was further verified by a significant release of DNA oxidation product, 8-hydroxydeoxyguanosine (8-OHdG), as well as by the Comet assay. For the in vivo study using the fruit fly D. melanogaster as a model, significant toxicity was observed in F1 progenies upon ingestion of ZnO NPs. ZnO NPs induced significant decrease in the egg-to-adult viability of the flies. We further showed that the decreased viability is closely associated with ROS induction by ZnO NPs. Removal of one copy of the D. melanogaster Nrf2 alleles further decreased the ZnO NPs-induced lethality due to increased production of ROS, indicating that nuclear factor E2-related factor 2 (Nrf2) plays important role in ZnO NPs-mediated ROS production. Conclusion The present study suggests that ZnO NPs induced significant oxidative stress-related cytotoxicity and genotoxicity in human lung fibroblasts in vitro and in D. melanogaster in vivo. More extensive studies would be needed to verify the safety issues related to increased usage of ZnO NPs by consumers.

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“…Therefore, it is difficult to predict the toxicological behavior of NPs in living organisms by in vitro models alone. 145,146 There are still many unanswered questions concerning nanoneurotoxicity. For instance, after bypassing the BBB, where do NPs go?…”

mentioning

confidence: 99%

Central nervous system toxicity of metallic nanoparticles

Feng¹,

Chen²,

Zhang³

et al. 2015

IJN

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Nanomaterials (NMs) are increasingly used for the therapy, diagnosis, and monitoring of disease- or drug-induced mechanisms in the human biological system. In view of their small size, after certain modifications, NMs have the capacity to bypass or cross the blood–brain barrier. Nanotechnology is particularly advantageous in the field of neurology. Examples may include the utilization of nanoparticle (NP)-based drug carriers to readily cross the blood–brain barrier to treat central nervous system (CNS) diseases, nanoscaffolds for axonal regeneration, nanoelectromechanical systems in neurological operations, and NPs in molecular imaging and CNS imaging. However, NPs can also be potentially hazardous to the CNS in terms of nano-neurotoxicity via several possible mechanisms, such as oxidative stress, autophagy, and lysosome dysfunction, and the activation of certain signaling pathways. In this review, we discuss the dual effect of NMs on the CNS and the mechanisms involved. The limitations of the current research are also discussed.

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Toxicity assessment of zinc oxide nanoparticles using sub-acute and sub-chronic murine inhalation models

Cited by 205 publications

References 49 publications

Significance of Intratracheal Instillation Tests for the Screening of Pulmonary Toxicity of Nanomaterials

Significance of Intratracheal Instillation Tests for the Screening of Pulmonary Toxicity of Nanomaterials

Zinc oxide nanoparticles exhibit cytotoxicity and genotoxicity through oxidative stress responses in human lung fibroblasts and <em>Drosophila melanogaster</em>

Central nervous system toxicity of metallic nanoparticles

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