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Spatiotemporal Distribution of Mesoporous Silica Nanoparticles in Tissue-Mimicking Collagen Using Lab-on-a-Chip Technology for Drug Carrier Diffusivity Evaluation

Title
Spatiotemporal Distribution of Mesoporous Silica Nanoparticles in Tissue-Mimicking Collagen Using Lab-on-a-Chip Technology for Drug Carrier Diffusivity Evaluation
Authors
Hwang, Hae WonKim, SeongchanHwang, HyerimHan, Hyung-SeopJeon, HojeongKim, Yu-ChanLee, HyojinSun, Jeong-YunOk, Myoung-Ryul
Ewha Authors
황혜림
SCOPUS Author ID
황혜림scopus
Issue Date
2022
Journal Title
ACS APPLIED NANO MATERIALS
ISSN
2574-0970JCR Link
Citation
ACS APPLIED NANO MATERIALS vol. 5, no. 9, pp. 12435 - 12443
Keywords
mesoporous silica nanoparticletransportationlab-on-a-chipdrug deliverydiffusion
Publisher
AMER CHEMICAL SOC
Indexed
SCIE; SCOPUS WOS scopus
Document Type
Article
Abstract
As injected drugs finally diffuse to the target cells, a quantitative understanding of the diffusion behavior of drug molecules or drug carriers is essential for the determination of their efficacy or optimal doses. Here, we propose a method for determining the diffusivity (D, diffusion coefficient) of drug carriers in tissue-mimicking collagen in the lab-on-a-chip (LOC) platform and predict their spatiotemporal distribution using the calculated D. By controlling the concentrations of fluorescent mesoporous silica nanoparticles (MSNs) in each channel, the diffusion of fluorescent MSNs was induced and fluorescence gradients in collagen were produced and captured as images. The D of the MSNs by size was obtained by fitting the fluorescence profiles to the solution of Fick's second law. The D of MSNs varied by size from 2.98 x 10-10 m2/s (MSNs of 10 nm) to 1.14 x 10-11 m2/s (MSNs of 1 mu m). The spatiotemporal profiles of MSNs were calculated using the obtained D, and it was demonstrated that the concentration of MSNs with a size > 200 nm at 100 mu m from the gel-liquid interface will remain < 50% of that in the vessel-mimicking channel even after 3 h. As the analysis and prediction procedures based on fluorescence profile image processing and a least-squares fit to the solution are relatively simple, our results can be extended to various studies to narrow the gap between in vitro tests and animal experiments in drug or particle transport research through the calculation of the diffusion coefficient of drug candidates before animal experiments and might replace some parts of animal experiments of drug delivery studies.
DOI
10.1021/acsanm.2c01936
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공과대학 > 화공신소재공학과 > Journal papers
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