Literature DB >> 30843265

Repeated oral dose toxicity study of nickel oxide nanoparticles in Wistar rats: a histological and biochemical perspective.

Naresh Dumala1,2, Bhanuramya Mangalampalli1,2, Sarika Srinivas Kalyan Kamal3, Paramjit Grover1,2.   

Abstract

Despite the increasing use of nickel oxide (NiO) nanoparticles (NPs), limited information is available on their toxicological effects. Health consequences of 28 days repeated oral exposure to NiO NPs have not been explored thoroughly. Hence, toxicity investigations were performed after 28-day daily exposure in albino Wistar rats with NiO NPs following Organization for Economic Co-operation and Development test guideline 407. Histopathology, biochemical indices including oxidative stress and biodistribution patterns were evaluated to decipher the toxicological impact of NiO NPs. NiO NP characterization by transmission electron microscopy showed an average size of 12.9 (±3.4) nm. Histological studies depicted a prominent impact on the vital organs of the rats. A dose-dependent rise in both aminotransferase enzyme values was recorded in the homogenates of liver and kidney tissues. A significant decrease in superoxide dismutase activity and increase in catalase activity was noted. Further, a dose-dependent decrease in reduced glutathione content was recorded in rats, which suggested generation of reactive oxygen species and oxidative stress. Increase in the malondialdehyde levels was observed with an increase in the dose substantiating the antioxidant enzyme activity profiles. Biodistribution studies indicated maximum accumulation of Ni content in liver followed by kidney. Excretion of Ni was predominantly through feces and a little through renal clearance. Our study indicated that NiO NPs adversely alter the biochemical profile of the rats and cause histological damage. Further investigations are warranted to address the mechanism by which physiological path these NiO NPs exhibit their toxic nature in in vivo.
© 2019 John Wiley & Sons, Ltd.

Entities:  

Keywords:  NiO nanoparticles; biodistribution of nickel; histopathology; oxidative stress; repeated dose 28-day oral toxicity study

Mesh:

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Year:  2019        PMID: 30843265     DOI: 10.1002/jat.3790

Source DB:  PubMed          Journal:  J Appl Toxicol        ISSN: 0260-437X            Impact factor:   3.446


  5 in total

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Authors:  Hoda S M Abdel-Ghany; Sobhy Abdel-Shafy; Mai M Abuowarda; Rabab M El-Khateeb; Essam Hoballah; Abdel Mohsen M Hammam; Magdy M Fahmy
Journal:  Exp Appl Acarol       Date:  2021-03-13       Impact factor: 2.132

2.  Hematobiochemical, Oxidative Stress, and Histopathological Mediated Toxicity Induced by Nickel Ferrite (NiFe2O4) Nanoparticles in Rabbits.

Authors:  Muhammad Shahid Khan; Saeed Ahmad Buzdar; Riaz Hussain; Gulnaz Afzal; Ghazala Jabeen; Muhammad Arshad Javid; Rehana Iqbal; Zahid Iqbal; Khola Bint Mudassir; Saba Saeed; Abdur Rauf; Hafiz Ishfaq Ahmad
Journal:  Oxid Med Cell Longev       Date:  2022-03-11       Impact factor: 6.543

3.  Peroral Toxicological Assessment of Two-Dimensional Forms of Nickel Nanoparticles Sized between 20 and 120 nm.

Authors:  Vladimir A Shipelin; Antonina A Shumakova; Eleonora N Trushina; Oksana K Mustafina; Alexander G Masyutin; Alexey I Kolobanov; Ilya E Sokolov; Ivan V Gmoshinski; Sergey A Khotimchenko; Dmitry B Nikityuk
Journal:  Nanomaterials (Basel)       Date:  2022-10-08       Impact factor: 5.719

4.  A metabolomic-based study on disturbance of bile acids metabolism induced by intratracheal instillation of nickel oxide nanoparticles in rats.

Authors:  Qiong Zhang; Xuhong Chang; Xiaoxia Wang; Haibing Zhan; Qing Gao; Mengmeng Yang; Han Liu; Sheng Li; Yingbiao Sun
Journal:  Toxicol Res (Camb)       Date:  2021-05-17       Impact factor: 3.524

Review 5.  Review and Evaluation of the Potential Health Effects of Oxidic Nickel Nanoparticles.

Authors:  Sharlee L More; Michael Kovochich; Tara Lyons-Darden; Michael Taylor; Alexandra M Schulte; Amy K Madl
Journal:  Nanomaterials (Basel)       Date:  2021-03-05       Impact factor: 5.076

  5 in total

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