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ToxSci Advance Access published online on July 2, 2009

Toxicological Sciences, doi:10.1093/toxsci/kfp139
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Published by Oxford University Press 2009.

Quantitative Determination of Skin Penetration of PEG-coated CdSe Quantum Dots in Dermabraded but not Intact SKH-1 Hairless Mouse Skin

Neera V. Gopeea,b, Dean W. Robertsa,b, Peggy Webba,b, Christy R. Cozarta, Paul H. Siitonena, John R. Latendressec, Alan R. Warbrittonc, William W. Yud, Vicki L. Colvind, Nigel J. Walkere and Paul C. Howarda,b,*

a National Center for Toxicological Research, U.S. Food & Drug Administration, Jefferson, AR 72079 b National Toxicology Program Center for Phototoxicology, U.S. Food & Drug Administration, Jefferson, AR 72079 c Toxicology Pathology Associates, Jefferson, AR 72079 d Center for Biological and Environmental Nanotechnology, Rice University, Houston, TX e National Toxicology Program, National Institute of Environmental Health Sciences, National Institutes of Health, Research Triangle Park, NC

* To whom correspondence should be addressed: Division of Biochemical Toxicology, National Toxicology Program Center for Phototoxicology, National Center for Toxicological Research, U.S. Food & Drug Administration, 3900 NCTR Rd, HFT-110, Jefferson, Arkansas 72079, Tel: (870)543-7672, or -7137, FAX: (870)543-7136, E-mail: Paul.Howard{at}fda.hhs.gov

Received March 15, 2009; revision received June 9, 2009; accepted June 18, 2009


   Abstract

Many cosmetics, sunscreens, and other consumer products are reported to contain nanoscale materials. The possible transdermal absorption of nanoscale materials and the long-term consequences of the absorption have not been determined. We used polyethylene glycol coated cadmium selenide (CdSe) core quantum dots (QD; 37 nm diameter) to evaluate the penetration of nanoscale material into intact, tape stripped, acetone treated, or dermabraded mouse skin. QD were suspended in an oil-in-water emulsion (approximately 9 µM) and the emulsion was applied at 2 mg/cm2 to mouse dorsal skin pretreated as follows: intact; tape-stripped to remove the stratum corneum; acetone pretreated; dermabraded to remove stratum corneum and epidermis. QD penetration into the skin was monitored in sentinel organs (liver and regional draining lymph nodes) using inductively coupled plasma mass spectrometry (ICP-MS) analysis of cadmium (from the CdSe QD). No consistent cadmium elevation was detected in the sentinel organs of mice with intact, acetone pretreated, or tape-stripped skin at 24 and 48 hr post QD application; however, in dermabraded mice, cadmium elevations were detected in the lymph nodes and liver. QD accumulation (as cadmium) in the liver was approximately 2.0% of the applied dose. The passing of QD through the dermabraded skin was confirmed using confocal fluorescence microscopy. These results suggest that transdermal absorption of nanoscale materials depends on skin barrier quality, and that the lack of an epidermis provided access to QD penetration. Future dermal risk assessments of nanoscale materials should consider key barrier aspects of skin and its overall physiologic integrity.

Key Words: quantum dots; nanoscale materials; dermabrasion.


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