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Alendronate-anionic clay nanohybrid for enhanced osteogenic proliferation and differentiation

Title
Alendronate-anionic clay nanohybrid for enhanced osteogenic proliferation and differentiation
Authors
Piao H.Kim M.H.Cui M.Choi G.Choy J.-H.
Ewha Authors
최진호최고은
SCOPUS Author ID
최진호scopus; 최고은scopus
Issue Date
2019
Journal Title
Journal of Korean Medical Science
ISSN
1011-8934JCR Link
Citation
Journal of Korean Medical Science vol. 34, no. 5
Keywords
AlendronateDrug delivery systemDrug-clay nanohybridInorganic delivery vehicleLayered double hydroxideOsteogenic proliferation and Differentiation
Publisher
Korean Academy of Medical Science
Indexed
SCIE; SCOPUS; KCI scopus
Document Type
Article
Abstract
Background: Alendronate (AL), a drug for inhibiting osteoclast-mediated bone-resorption, was intercalated into an inorganic drug delivery nanovehicle, layered double hydroxide (LDH), to form a new nanohybrid, AL-LDH, with 1:1 heterostructure along the crystallographic C-axis. Based on the intercalation reaction strategy, the present AL-LDH drug delivery system (DDS) was realized with an enhanced drug efficacy of AL, which was confirmed by the improved proliferation and osteogenic differentiation of osteoblast-like cells (MG63). Methods: The AL-LDH nanohybrid was synthesized by conventional ion-exchange reaction and characterized by powder X-ray diffraction (PXRD), high-resolution transmission electron microscopy (HR-TEM), and Fourier transform infrared (FT-IR) spectroscopy. Additionally, in vitro efficacy tests, such as cell proliferation and alkaline phosphatase (ALP) activity, were analyzed. Results: The AL was successfully intercalated into LDH via ion-exchange reaction, and thus prepared AL-LDH DDS was X-ray single phasic and chemically well defined. The accumulated AL content in MG63 cells treated with the AL-LDH DDS nanoparticles was determined to be 10.6-fold higher than that within those treated with the intact AL after incubation for 1 hour, suggesting that intercellular permeation of AL was facilitated thanks to the hybridization with drug delivery vehicle, LDH. Furthermore, both in vitro proliferation level and ALP activity of MG63 treated with the present hybrid drug, AL-LDH, were found to be much more enhanced than those treated with the intact AL. This is surely due to the fact that LDH could deliver AL drug very efficiently, although LDH itself does not show any effect on proliferation and osteogenic differentiation of MG63 cells. Conclusion: The present AL-LDH could be considered as a promising DDS for improving efficacy of AL. © 2019 The Korean Academy of Medical Sciences.
DOI
10.3346/jkms.2019.34.e37
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자연과학대학 > 화학·나노과학전공 > Journal papers
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