9 7 6 4 1
论文已发表
注册即可获取德孚的最新动态
IF 收录期刊
- 3.3 Breast Cancer (Dove Med Press)
- 3.4 Clin Epidemiol
- 2.5 Cancer Manag Res
- 2.9 Infect Drug Resist
- 3.5 Clin Interv Aging
- 4.7 Drug Des Dev Ther
- 2.7 Int J Chronic Obstr
- 6.6 Int J Nanomed
- 2.5 Int J Women's Health
- 2.5 Neuropsych Dis Treat
- 2.7 OncoTargets Ther
- 2.0 Patient Prefer Adher
- 2.3 Ther Clin Risk Manag
- 2.5 J Pain Res
- 2.8 Diabet Metab Synd Ob
- 2.8 Psychol Res Behav Ma
- 3.0 Nat Sci Sleep
- 1.8 Pharmgenomics Pers Med
- 2.7 Risk Manag Healthc Policy
- 4.2 J Inflamm Res
- 2.1 Int J Gen Med
- 4.2 J Hepatocell Carcinoma
- 3.7 J Asthma Allergy
- 1.9 Clin Cosmet Investig Dermatol
- 2.7 J Multidiscip Healthc
A comparison of poly-ethylene-glycol-coated and uncoated gold nanoparticle-mediated hepatotoxicity and oxidative stress in Sprague Dawley rats
Authors Patlolla AK, Kumari SA, Tchounwou PB
Received 31 August 2018
Accepted for publication 10 November 2018
Published 15 January 2019 Volume 2019:14 Pages 639—647
DOI https://doi.org/10.2147/IJN.S185574
Checked for plagiarism Yes
Review by Single-blind
Peer reviewers approved by Dr Govarthanan Muthusamy
Peer reviewer comments 2
Editor who approved publication: Dr Thomas J Webster
Background: Gold nanoparticles (GNPs) and their
functional derivatives are of great interest because of their many biomedical
applications. GNPs are increasingly being incorporated into new diagnostic and
therapeutic approaches in medicine. Consequently, there has been a strong push
to fully understand their interactions with blood components. The agglomeration
of cells reflects the interaction of nanoparticles with blood components.
Methods: The
main aim of this study was to compare the effects of poly-ethylene-glycol
(PEG)-oated and uncoated GNPs on the generation of reactive oxygen species
(ROS); on the actions of distinct hepatotoxicity biomarkers such as alanine
(ALT) and aspartate (AST) aminotransferases, and alkaline phosphatase (ALP);
and on the histology of liver tissues in the rat model. Four distinct doses of
PEG-coated and uncoated GNPs (12.5, 25, 50, and 100 µg/kg body weight) were
used. Each group consisted of three rats receiving an oral administration of
PEG-coated and uncoated GNPs for 5 days with one dose per 24 hours. The
control group consisted of three rats that received deionized water.
Twenty-four hours after the last treatment, samples were collected following
standard procedures.
Results: PEG-coated
and uncoated GNPs enhanced the generation of ROS and the activity of serum
aminotransferases (ALT/AST) and ALPs relative to the negative control. A liver
histology assessment of GNP-exposed rats revealed statistically significant
responses in the variation of the morphologies of tissues relative to those of
the negative control. Nonetheless, uncoated GNPs demonstrated enhanced
hepatotoxic outcomes relative to those of PEG-coated GNPs. The results
demonstrated that both GNPs may be able to promote hepatotoxicity in Sprague Dawley
rats through mechanisms of oxidative stress. However, uncoated GNPs have more
harmful effects than PEG-coated GNPs relative to the negative control.
Conclusion: Taken
together, the results of this study indicate that PEG-coated GNPs may be safer
to use in nanomedicinal applications than uncoated GNPs. However, more studies
must be performed to confirm the outcomes of PEGylation.
Keywords: serum
aminotransferases, polyethylene glycol coated gold nanoparticles, uncoated gold
nanoparticles, hepatotoxicity, oxidative stress
摘要视频链接:PEG-coated and
uncoated GNP-mediated hepatotoxicity and oxidative stress
