Issue 23, 2012
From the journal:

Nanoscale

Capacity of mesoporous bioactive glass nanoparticles to deliver therapeutic molecules

Ahmed El-Fiqi,abc   Tae-Hyun Kim,ab   Meeju Kim,ab   Mohamed Eltohamy,abc   Jong-Eun Won,ab   Eun-Jung Leeab  and  Hae-Won Kim*abcd  

* Corresponding authors

a Department of Nanobiomedical Science and WCU Research Center, Dankook University, South Korea

b Institute of Tissue Regeneration Engineering (ITREN), Dankook University, South Korea
E-mail: kimhw@dku.edu
Fax: +82 41 550 3085
Tel: +82 41 550 3081

c Glass Research Department, National Research Center, Egypt

d Department of Biomaterials Science, School of Dentistry, Dankook University, South Korea

Abstract

Inorganic bioactive nanomaterials are attractive for hard tissue regeneration, including nanocomponents for bone replacement composites and nanovehicles for delivering therapeutics. Bioactive glass nanoparticles (BGn) have recently gained potential usefulness as bone and tooth regeneratives. Here we demonstrate the capacity of the BGn with mesopores to load and deliver therapeutic molecules (drugs and particularly genes). Spherical BGn with sizes of 80–90 nm were produced to obtain 3–5 nm sized mesopores through a sono-reacted sol–gel process. A simulated body fluid test of the mesoporous BGn confirmed their excellent apatite forming ability and the cellular toxicity study demonstrated their good cell viability up to 100 μg ml−1. Small molecules like chemical drug (Na-ampicillin) and gene (small interfering RNA; siRNA) were introduced as model drugs considering the mesopore size of the nanoparticles. Moreover, amine-functionalization allowed switchable surface charge property of the BGn (from −20–30 mV to +20–30 mV). Loading of ampicillin or siRNA saturated within a few hours (∼2 h) and reflected the mesopore structure. While the ampicillin released relatively rapidly (∼12 h), the siRNA continued to release up to 3 days with almost zero-order kinetics. The siRNA–nanoparticles were easily taken up by the cells, with a transfection efficiency as high as ∼80%. The silencing effect of siRNA delivered from the BGn, as examined by using bcl-2 model gene, showed dramatic down-regulation (∼15% of control), suggesting the potential use of BGn as a new class of nanovehicles for genes. This, in conjunction with other attractive properties, including size- and mesopore-related high surface area and pore volume, tunable surface chemistry, apatite-forming ability, good cell viability and the possible ion-related stimulatory effects, will potentiate the usefulness of the BGn in hard tissue regeneration.

Graphical abstract: Capacity of mesoporous bioactive glass nanoparticles to deliver therapeutic molecules

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Article information

DOI
https://doi.org/10.1039/C2NR31775C
Article type
Paper
Submitted
08 Jul 2012
Accepted
06 Oct 2012
First published
09 Oct 2012

Nanoscale, 2012,4, 7475-7488

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Capacity of mesoporous bioactive glass nanoparticles to deliver therapeutic molecules

A. El-Fiqi, T. Kim, M. Kim, M. Eltohamy, J. Won, E. Lee and H. Kim, Nanoscale, 2012, 4, 7475 DOI: 10.1039/C2NR31775C

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