4.7 Article

Analysis of model drug permeation through highly crosslinked and biodegradable polyethylene glycol membranes

期刊

JOURNAL OF MEMBRANE SCIENCE
卷 645, 期 -, 页码 -

出版社

ELSEVIER
DOI: 10.1016/j.memsci.2021.120218

关键词

Drug permeation; Biodegradable membrane; Multiarm polyethylene glycol; Lyophilized membrane

资金

  1. JSPS KAKENHI [17H03464, 21J12280]
  2. Grants-in-Aid for Scientific Research [17H03464, 21J12280] Funding Source: KAKEN

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Biodegradable PEG membranes were developed for sustained drug release in the body, demonstrating biodegradability and drug permeability.
Various natural and synthetic polymers, such as hyaluronan and functionalized polyethylene glycol (PEG), have been used to fabricate biodegradable membranes. They can potentially be used for local drug release in the body because of their biodegradability. However, this biodegradability causes to difficulties in sustained drug release, and an insufficient ability to control drug permeability can lead to adverse effects. In this study, we developed biodegradable lyophilized PEG membranes from highly crosslinked PEG hydrogels to control drug permeation. Three-arm thiol-modified PEG (PEG-SH, molecular weight [M-w] = 1300) and four-arm acrylate-modified PEG (PEG-AC, M-w = 1892) were used to fabricate the PEG hydrogels, which were then lyophilized to obtain PEG membranes. The degradation time of these PEG membranes was 25 days under physiological conditions. Despite their biodegradability, the membranes allowed the permeation of model drugs constantly until complete degradation around physiological pH. The normalized diffusion coefficients (ln[D/D-0]) for vitamin B12 and lysozyme (Lys) were -2.6 and -4.8, respectively. In addition, the membranes showed biodegradability and biocompatibility in the abdominal cavity of mice. These results indicate that PEG membranes can be used for sustained drug release in the body due to their biodegradability and drug permeability.

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