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Neelesh R. Soman, Steven L. Baldwin, Grace Hu, Jon N. Marsh, Gregory M. Lanza, John E. Heuser, Jeffrey M. Arbeit, Samuel A. Wickline, Paul H. Schlesinger
Published in Volume 119, Issue 9
J Clin Invest. 2009; 119(9):2830–2842 doi:10.1172/JCI38842
Abstract | Full text | PDF
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Figure 7
Regression of precancerous epidermal dysplatic lesions in the ears of K14-HPV16 mice by αvβ3 integrin–targeted melittin-loaded nanoparticles.

(A) Fluorescence microscopy pictures of mouse ear sections showing the extensive overlay with FITC-lectin (shown by arrows) of αvβ3 integrin–targeted rhodamine-nanoparticles compared with nontargeted ones. (B) Representative H&E-stained pictures of K14-HPV16 mouse ear sections after treatment with 7 doses of melittin-loaded nanoparticles (melittin dose, 13 mg/kg). Note the regression of papillae (shown by arrows) in the group treated with αvβ3 integrin–targeted melittin-loaded nanoparticles. Scale bars: 100 μm (C) Chart showing the specific effect of targeted melittin-loaded nanoparticles on regression of severe papillae (greater than 100 μm). Data are represented as mean ± SEM. n = 5. *P < 0.05.