期刊
BIOMATERIALS SCIENCE
卷 9, 期 11, 页码 4169-4177出版社
ROYAL SOC CHEMISTRY
DOI: 10.1039/d1bm00135c
关键词
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资金
- Fundamental Research Funds for the Central Universities [2232021G-04]
- Shanghai Pujiang Program [2019PJD002]
- Shanghai Natural Science Foundation [18ZR1401800]
Injectable hydrogels based on keratin and Au(iii) salt were developed through dynamic exchange between disulfide bonds (S-S) and gold(i)-thiolates (Au-S). This hydrogel showed a good hemostatic effect and was efficient as a drug loading carrier, demonstrating desirable wound healing effects in various models.
Injectable hydrogels hold promise in biomedical applications due to their noninvasive administration procedure and capacity enabling the filling of irregularly shaped defects. Protein-based hydrogels provide features including good biocompatibility and inherent biofunction. However, challenges still remain to develop a protein-based injectable hydrogel in a convenient way due to the limited active groups in proteins. Keratins are a group of cysteine-rich structural proteins found abundantly in skin and skin appendages. In this work, we utilized keratin and the Au(iii) salt to develop an injectable hydrogel based on the dynamic exchange between disulfide bonds (S-S) and gold(i)-thiolates (Au-S). Such a hydrogel could be prepared at the physiological pH and applied as an injectable hydrogel for biomedical applications including hemostatic and wound dressing materials. Our findings demonstrated that this keratin injectable hydrogel showed a good hemostatic effect in both tail amputation and liver injury models. Moreover, it was proved efficient as a drug loading carrier, and the deferoxamine-loaded hydrogel showed a desirable wound healing effect in a full-thickness excision wound model.
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