4.7 Article

New Polyvinyl Alcohol/Succinoglycan-Based Hydrogels for pH-Responsive Drug Delivery

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POLYMERS
卷 15, 期 14, 页码 -

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MDPI
DOI: 10.3390/polym15143009

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succinoglycan; polyvinyl alcohol; freeze-thaw; hydrogel; pH-responsive drug delivery

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In this study, new hydrogels were fabricated using polyvinyl alcohol (PVA) and succinoglycan (SG) obtained from Sinorhizobium meliloti Rm 1021. The hydrogel composition and freeze-thaw cycles were optimized to enhance the swelling ratio. The optimized hydrogel exhibited pH-responsive drug release and was non-toxic and biocompatible, making it a potential candidate for chronic wound dressing applications.
We fabricated new hydrogels using polyvinyl alcohol (PVA) and succinoglycan (SG) directly isolated and obtained from Sinorhizobium meliloti Rm 1021 via the freeze-thaw method. Both the composition of the hydrogels and the freeze-thaw cycles were optimized to maximize the swelling ratio for the preparation of the PVA/SG hydrogels. During the optimization process, the morphology and conformational change in the hydrogel were analyzed by scanning electron microscopy, rheological measurements, and compressive tests. An optimized hydrogel with a maximum swelling ratio of 17.28 g/g was obtained when the composition of PVA to SG was 50:50 (PVA/SG 50/50) and the total number of freeze-thaw cycles was five. The PVA/SG 50/50 hydrogel had the largest pore with 51.24% porosity and the highest cross-over point (28.17%) between the storage modulus (G & PRIME;) and the loss modulus (G & DPRIME;). The PVA/SG 50/50 hydrogel showed improved thermal stability owing to its interaction with thermally stable SG chains. The improvement in the thermal stability was confirmed by thermogravimetric analysis and differential scanning calorimetry. In addition, the PVA/SG 50/50 hydrogel showed differential drug release according to the corresponding pH under acidic conditions of pH 1.2 and slightly basic conditions of pH 7.4. Furthermore, the cell viability test on the HEK-293 cell line for that hydrogel demonstrated that the PVA/SG 50/50 hydrogel was non-toxic and biocompatible. Therefore, this hydrogel could be a potential scaffold capable of pH-responsive drug delivery for chronic wound dressing applications.

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