Synthesis of transdermal aloesin loaded zinc oxide nanoparticles and its inhibitory effect on the activity of tyrosinase.

Xiao Huang; Chun Chen; Xingquan Gong; Zuli Xiao; Xiulan Shi; Xi Zheng; Yuzhu Pan; Caixia YI

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Synthesis of transdermal aloesin loaded zinc oxide nanoparticles and its inhibitory effect on the activity of tyrosinase.

Author: Xiao HUANG ¹ ; Chun CHEN ² ; Xingquan GONG ² ; Zuli XIAO ² ; Xiulan SHI ¹ ; Xi ZHENG ¹ ; Yuzhu PAN ³ ; Caixia YI ⁴
Author Information

1. School of Sports and Health Science, Tongren University, Tongren, Guizhou 554300, P.R.China.
2. College of Material and Chemical Engineering, Tongren University, Tongren, Guizhou 554300, P.R.China.
3. Chongqing Mix Biotechnology co., Ltd., Chongqing 400039, P.R.China.
4. School of Sports and Health Science, Tongren University, Tongren, Guizhou 554300, P.R.China.465086552@qq.com.
Publication Type:Journal Article
Keywords: aloesin; controlled release; transdermal delivery; tyrosinase inhibitor; zinc oxide quantum dots
MeSH: Administration, Cutaneous; Animals; Chromones; administration & dosage; Drug Delivery Systems; Glucosides; administration & dosage; Guinea Pigs; Monophenol Monooxygenase; metabolism; Nanoparticles; Quantum Dots; Zinc Oxide
From: Journal of Biomedical Engineering 2019;36(2):254-259
CountryChina
Language:Chinese
Abstract: Zinc oxide quantum dots (ZnO QDs) were synthesized by gel-sol method and employed as the transdermal aloesin (Alo) carriers. ZnO QDs were surface-functionalized with amino using aminopropyltriethoxysilane (APTES). Alo was covalently bonded on the surface of ZnO QDs via N,N'-carbonyldiimidazole to obtain Alo NPs, which were characterized by transmission electron microscope (TEM), dynamic light scattering (DLS), Fourier transform infrared spectroscopy (FTIR) and thermal gravimetric analyzer (TGA). TEM images showed that ZnO QDs were analogously sphere and monodisperse with a reasonably narrow size distribution, of which was around 4 nm. The size of Alo NPs increased to around 8 nm due to the surface modification. The intense bands at around 3 400 cm and 1 200 cm in the FTIR spectrum of Alo NPs from the vibration of -OH indicated the linkage of Alo on the surface of ZnO QDs. The results of TGA analysis showed that the mass ratio of ZnO QDs and Alo were 39.27% and 35.14%, respectively. The penetration of Alo NPs was much higher than raw Alo according to the passive penetration experiments with Franz-type diffusion cells instrument using full-thickness cavy skin, which manifested the improvement of the penetration for Alo delivered by ZnO QDs. The pH-controlled drug release behavior was investigated. At pH 7.4, only a small amount of Alo (1.45% ± 0.21%) had been released after 2 h. In contrast, as incubation at pH 5.0 of which pH was similar to endosomal environment, Alo was released very fast (87.63% ± 0.46% in 2 h) from Alo NPs, confirming that Alo NPs could response to the pH and realize the intracellular drug release. The inhibitory effect of Alo NPs on tyrosinase was in a dose dependent manner. When the concentration of Alo NPs was 12.5 μg/mL, the inhibition rate was up to 40.32% ± 1.57%. All the results show that the Alo NPs hold a great potential in transdermal tyrosinase inhibition.