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Assessing Clinical Prospects of Silicon Quantum Dots: Studies in Mice and Monkeys

Authors
Liu, JianweiErogbogbo, FolarinYong, Ken-TyeYe, LingLiu, JingHu, RuiChen, HongyanHu, YazhuoYang, YiYang, JinghuiRoy, IndrajitKarker, Nicholas A.Swihart, Mark T.Prasad, Paras N.
Issue Date
8월-2013
Publisher
AMER CHEMICAL SOC
Keywords
quantum dots; silicon; toxicity; in vivo; nanocrystals
Citation
ACS NANO, v.7, no.8, pp.7303 - 7310
Indexed
SCIE
SCOPUS
Journal Title
ACS NANO
Volume
7
Number
8
Start Page
7303
End Page
7310
URI
https://scholar.korea.ac.kr/handle/2021.sw.korea/102584
DOI
10.1021/nn4029234
ISSN
1936-0851
Abstract
Silicon nanocrystals can provide the outstanding imaging capabilities of toxic heavy-metal-based quantum dots without employing heavy metals and have potential for rapid progression to the clinic. Understanding the toxicity of silicon quantum dots (SiQDs) is essential to realizing this potential. However, existing studies of SiQD biocompatibility are limited, with no systematic progression from small-animal to large-animal studies that are more clinically relevant. Here, we test the response of both mice and monkeys to high intravenous doses of a nanoconstruct created using only SiQDs and FDA-approved materials. We show that (1) neither mice nor monkeys show overt signs of toxicity reflected in their behavior, body mass, or blood chemistry, even at a dose of 200 mg/kg. (2) This formulation did not biodegrade as expected. Elevated levels of silicon were present in the liver and spleen of mice three months post-treatment. (3) Histopathology three months after treatment showed adverse effects of the nanoformulation in the livers of mice, but showed no such effects in monkeys. This investigation reveals that the systemic reactions of the two animal models may have some differences and there are no signs of toxicity clearly attributable to silicon quantum dots.
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