Persistent Hepatic Structural Alterations Following Nanoceria Vascular Infusion in the Rat

Tseng, Michael T.; Fu, Qiang; Lor, Khoua; Fernandez-Botran, G. Rafael; Deng, Zhongbin; Graham, Uschi M.; Butterfield, D. Allan; Grulke, Eric A.; Yokel, Robert A.

doi:10.1177/0192623313505780

Cited by 23 publications

(27 citation statements)

References 40 publications

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“…A 30 nm ceria showed similar Ce 3+ enrichment on its surface. Its core had a greater percentage of Ce 4+ 18, 38 . These results did not show nanoceria biotransformation over this short time.…”

Section: Systemic Nanoceria Exposurementioning

confidence: 99%

“…Intravenous infusion of 85 mg/kg of a 30 nm ceria produced nanoceria-laden Kupffer cells. These stimulated CD3 + lymphocyte proliferation in the sinusoids to form granulomata, composed of ceria-laden Kupffer cells and a few non-ceria accumulating mononuclear cells, that were seen 30 days after the single nanoceria dose and persisted without great resolution or progression to 90 days after dosing 18, 38 . The granuloma were of the non-necrotizing type and did not progress to frank hepatic necrosis.…”

Section: Systemic Nanoceria Exposurementioning

confidence: 99%

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The yin: an adverse health perspective of nanoceria: uptake, distribution, accumulation, and mechanisms of its toxicity

Yokel

Hussain

Garantziotis

et al. 2014

Environ. Sci.: Nano

Self Cite

104

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This critical review evolved from a SNO Special Workshop on Nanoceria panel presentation addressing the toxicological risks of nanoceria: accumulation, target organs, and issues of clearance; how exposure dose/concentration, exposure route, and experimental preparation/model influence the different reported effects of nanoceria; and how can safer by design concepts be applied to nanoceria? It focuses on the most relevant routes of human nanoceria exposure and uptake, disposition, persistence, and resultant adverse effects. The pulmonary, oral, dermal, and topical ocular exposure routes are addressed as well as the intravenous route, as the latter provides a reference for the pharmacokinetic fate of nanoceria once introduced into blood. Nanoceria reaching the blood is primarily distributed to mononuclear phagocytic system organs. Available data suggest nanoceria’s distribution is not greatly affected by dose, shape, or dosing schedule. Significant attention has been paid to the inhalation exposure route. Nanoceria distribution from the lung to the rest of the body is less than 1% of the deposited dose, and from the gastrointestinal tract even less. Intracellular nanoceria and organ burdens persist for at least months, suggesting very slow clearance rates. The acute toxicity of nanoceria is very low. However, large/accumulated doses produce granuloma in the lung and liver, and fibrosis in the lung. Toxicity, including genotoxicity, increases with exposure time; the effects disappear slowly, possibly due to nanoceria’s biopersistence. Nanoceria may exert toxicity through oxidative stress. Adverse effects seen at sites distal to exposure may be due to nanoceria translocation or released biomolecules. An example is elevated oxidative stress indicators in the brain, in the absence of appreciable brain nanoceria. Nanoceria may change its nature in biological environments and cause changes in biological molecules. Increased toxicity has been related to greater surface Ce3+, which becomes more relevant as particle size decreases and the ratio of surface area to volume increases. Given its biopersistence and resulting increased toxicity with time, there is a risk that long-term exposure to low nanoceria levels may eventually lead to adverse health effects. This critical review provides recommendations for research to resolve some of the many unknowns of nanoceria’s fate and adverse effects.

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Section: Systemic Nanoceria Exposurementioning

confidence: 99%

Section: Systemic Nanoceria Exposurementioning

confidence: 99%

The yin: an adverse health perspective of nanoceria: uptake, distribution, accumulation, and mechanisms of its toxicity

Yokel

Hussain

Garantziotis

et al. 2014

Environ. Sci.: Nano

Self Cite

104

View full text Add to dashboard Cite

show abstract

“…Previous studies have shown that CeO 2 nanoparticles in therapeutic doses are non-toxic [14], relatively stable and accumulate in liver upon intravenous injection [15]. While some studies demonstrated toxicity of CeO 2 nanoparticles in high doses [16], it has now been shown that the toxicity is based on whether the particles exist in Ce +3 or Ce +4 and the relative ratio of Ce +3 /Ce +4 [17]. Furthermore, several studies have shown that CeO 2 nanoparticles can be used to treat stroke [18], ovarian cancer [19], cardiomyopathy [20], sepsis [21] and obesity [22].…”

Section: Introductionmentioning

confidence: 99%

Prophylactic Treatment with Cerium Oxide Nanoparticles Attenuate Hepatic Ischemia Reperfusion Injury in Sprague Dawley Rats

Manne¹,

Arvapalli

Graffeo³

et al. 2017

Cell Physiol Biochem

553

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Background: Hepatic ischemia reperfusion is one the main causes for graft failure following transplantation. Although, the molecular events that lead to hepatic failure following ischemia reperfusion (IR) are diverse and complex, previous studies have shown that excessive formation of reactive oxygen species (ROS) are responsible for hepatic IR injury. Cerium oxide (CeO 2 ) nanoparticles have been previously shown to act as an anti-oxidant and anti-inflammatory agent. Here, we evaluated the protective effects of CeO 2 nanoparticles on hepatic ischemia reperfusion injury. Methods: Male Sprague Dawley rats were randomly assigned to one of the four groups: Control, CeO 2 nanoparticle only, hepatic ischemia reperfusion (IR) group and hepatic ischemia reperfusion (IR) plus CeO 2 nanoparticle group (IR+ CeO 2 ). Partial warm hepatic ischemia was induced in left lateral and median lobes for 1h, followed by 6h of reperfusion. Animals were sacrificed after 6h of reperfusion and blood and tissue samples were collected and processed for various biochemical experiments. Results: Prophylactic treatment with CeO 2 nanoparticles (0.5mg/kg i.v (IR+CeO 2 group)) 1 hour prior to hepatic ischemia and subsequent reperfusion injury lead to a decrease in serum levels of alanine aminotransaminase and lactate dehydrogenase at 6 hours after reperfusion. These changes were accompanied by significant decrease in hepatocyte necrosis along with reduction in several serum inflammatory markers such as macrophage derived chemokine, macrophage inflammatory protein-2, KC/GRO, myoglobin and plasminogen activator inhibitor-1. However, immunoblotting demonstrated no significant changes in the levels of apoptosis related protein markers such as bax, bcl2 and caspase 3 in IR and IR+ CeO2 groups at 6 hours suggesting necrosis as the main pathway for hepatocyte death. Conclusion: Taken together, these data suggest that CeO 2 nanoparticles attenuate IR induced cell death and can be used as a prophylactic agent to prevent hepatic injury associated with graft failure.Room 315,

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“…[17] When ceria nanoparticles (CeO 2 NPs) are sequestered in a rat liver, cytotoxicity occurs, as evidenced by hepatocyte enlargement, sinusoidal dilatation, accumulation of Kupffer cells, and formation of granuloma. [18, 19] In fact, it was recently shown that CeO 2 NPs uptake by the liver also coincides with early pro-oxidant effects in the rat brain, [20] which is followed by a transition to oxidative stress and then, unexpectedly, reverses back to no stress after ninety days. [21] Despite substantial studies that have focused on CeO 2 NPs uptake, distribution, and biopersistance, [1–4,22, 23] so far, no information has been available on its chemical and structural stability once sequestered inside the liver, the organ that stores the greatest amount of CeO 2 NPs.…”

Section: Introductionmentioning

confidence: 99%

In Vivo Processing of Ceria Nanoparticles inside Liver: Impact on Free‐Radical Scavenging Activity and Oxidative Stress

et al. 2014

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The cytotoxicity of ceria ultimately lies in its electronic structure, which is defined by the crystal structure, composition, and size. Despite previous studies focused on ceria uptake, distribution, biopersistance, and cellular effects, little is known about its chemical and structural stability and solubility once sequestered inside the liver. Mechanisms will be presented that elucidate the in vivo transformation in the liver. In vivo processed ceria reveals a particle-size effect towards the formation of ultrafines, which represent a second generation of ceria. A measurable change in the valence reduction of the second-generation ceria can be linked to an increased free-radical scavenging potential. The in vivo processing of the ceria nanoparticles in the liver occurs in temporal relation to the brain cellular and protein clearance responses that stem from the ceria uptake. This information is critical to establish a possible link between cellular processes and the observed in vivo transformation of ceria. The temporal linkage between the reversal of the pro-oxidant effect (brain) and ceria transformation (liver) suggests a cause–effect relationship.

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Persistent Hepatic Structural Alterations Following Nanoceria Vascular Infusion in the Rat

Cited by 23 publications

References 40 publications

The yin: an adverse health perspective of nanoceria: uptake, distribution, accumulation, and mechanisms of its toxicity

The yin: an adverse health perspective of nanoceria: uptake, distribution, accumulation, and mechanisms of its toxicity

Prophylactic Treatment with Cerium Oxide Nanoparticles Attenuate Hepatic Ischemia Reperfusion Injury in Sprague Dawley Rats

In Vivo Processing of Ceria Nanoparticles inside Liver: Impact on Free‐Radical Scavenging Activity and Oxidative Stress

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