Assessment of genotoxicity and biodistribution of nano‐ and micron‐sized yttrium oxide in rats after acute oral treatment

Panyala, Archana; Chinde, Srinivas; Kumari, Sushma; Grover, Paramjit

doi:10.1002/jat.3505

Cited by 12 publications

(3 citation statements)

References 61 publications

(70 reference statements)

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“…These studies included a single oral exposure with female Wistar rats, and a 28-day repeated oral exposure study with both male and female Wistar rats. Comet and MN assays for liver and peripheral blood erythrocytes, respectively, were all positive in rats treated with a single dose of Y 2 O 3 , and both single and repeated dose of WO 3 at the highest tested dose (1000 mg/kg body weight) [ 68 – 70 ]. In rats treated with a repeated dose of Y 2 O 3 , all tests were positive already at 120–480 mg/kg body weight [ 71 ].…”

Section: Literature Quality Evaluation Resultsmentioning

confidence: 99%

A systematic quality evaluation and review of nanomaterial genotoxicity studies: a regulatory perspective

et al. 2022

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The number of publications in the field of nanogenotoxicology and the amount of genotoxicity data on nanomaterials (NMs) in several databases generated by European Union (EU) funded projects have increased during the last decade. In parallel, large research efforts have contributed to both our understanding of key physico-chemical (PC) parameters regarding NM characterization as well as the limitations of toxicological assays originally designed for soluble chemicals. Hence, it is becoming increasingly clear that not all of these data are reliable or relevant from the regulatory perspective. The aim of this systematic review is to investigate the extent of studies on genotoxicity of NMs that can be considered reliable and relevant by current standards and bring focus to what is needed for a study to be useful from the regulatory point of view. Due to the vast number of studies available, we chose to limit our search to two large groups, which have raised substantial interest in recent years: nanofibers (including nanotubes) and metal-containing nanoparticles. Focusing on peer-reviewed publications, we evaluated the completeness of PC characterization of the tested NMs, documentation of the model system, study design, and results according to the quality assessment approach developed in the EU FP-7 GUIDEnano project. Further, building on recently published recommendations for best practices in nanogenotoxicology research, we created a set of criteria that address assay-specific reliability and relevance for risk assessment purposes. Articles were then reviewed, the qualifying publications discussed, and the most common shortcomings in NM genotoxicity studies highlighted. Moreover, several EU projects under the FP7 and H2020 framework set the aim to collectively feed the information they produced into the eNanoMapper database. As a result, and over the years, the eNanoMapper database has been extended with data of various quality depending on the existing knowledge at the time of entry. These activities are highly relevant since negative results are often not published. Here, we have reviewed the NanoInformaTIX instance under the eNanoMapper database, which hosts data from nine EU initiatives. We evaluated the data quality and the feasibility of use of the data from a regulatory perspective for each experimental entry.

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Section: Literature Quality Evaluation Resultsmentioning

confidence: 99%

A systematic quality evaluation and review of nanomaterial genotoxicity studies: a regulatory perspective

et al. 2022

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“…When this paper (Panyala et al, 2017) was first published, there was a problem with Figure 2. The caption stated that Figure 2G,I showed the normal architecture of the heart and spleen and that Figure 2H,J showed that there was no pathological alterations in the heart and spleen of the Y2 O3 NO‐treated group.…”

Section: Figurementioning

confidence: 99%

Assessment of genotoxicity and biodistribution of nano‐ and micron‐sized yttrium oxide in rats after acute oral treatment

Panyala¹,

Chinde²,

Kumari³

et al. 2022

J of Applied Toxicology

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“…Following ingestion, translocation of particles into and across the GIT mucosa can occur via four mechanisms: 1) endocytosis, through enterocytes, 2) the M-cell-rich layer of Peyer's patches (small-intestine lymphoid aggregates), 3) persorption, where particles can translocate through a "hole" left in the epithelium when enterocytes shed from the villous tip, and 4) the paracellular route, where NPs pass through weakened tight junctions of the epithelial cell layer. [17][18][19][20] Moreover, NP translocation and interactions with tissues in the GIT can be influenced by size, morphology, hydrophilic-hydrophobic balance, and surface functionalization of the particles in question. For example, it has been suggested that negatively charged materials exhibit poor bioavailability, due to electrostatic repulsion and mucus entrapment.…”

Section: Introductionmentioning

confidence: 99%

Nanodelivery systems and stabilized solid-drug nanoparticles for orally administered medicine: current landscape

Kermanizadeh¹,

Powell²,

Stone³

2018

IJN

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The use of nanoparticles as a means of targeted delivery of therapeutics and imaging agents could greatly enhance the transport of biologically active contents to specific target tissues, while avoiding or reducing potentially undesired side effects. Generally speaking, the oral route of administration is associated with good patient compliance, as it is convenient, economical, noninvasive, and does not require special training. Here, we review the progress of the utilization of nanodelivery-system carriers or stabilized solid-drug nanoparticles following oral administration, with particular attention on toxicological data. Mechanisms of cytotoxicity are discussed and the problem of extrapolating knowledge to human scenarios highlighted. Additionally, issues associated with administration of drugs via the oral route are underlined, while strategies utilized to overcome these are highlighted. This review aims to offer a balanced overview of strategies currently being used in the application of nanosize constructs for oral medical applications.

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Assessment of genotoxicity and biodistribution of nano‐ and micron‐sized yttrium oxide in rats after acute oral treatment

Cited by 12 publications

References 61 publications

A systematic quality evaluation and review of nanomaterial genotoxicity studies: a regulatory perspective

A systematic quality evaluation and review of nanomaterial genotoxicity studies: a regulatory perspective

Assessment of genotoxicity and biodistribution of nano‐ and micron‐sized yttrium oxide in rats after acute oral treatment

Nanodelivery systems and stabilized solid-drug nanoparticles for orally administered medicine: current landscape

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