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用于递送人脂联素治疗小鼠溃疡性结肠炎的基因工程丝胶蛋白水凝胶

Genetically engineered sericin hydrogels for the delivery of human adiponectin in treating ulcerative colitis in mice.

作者信息

Zhou Hongji, Zhou Yujuan, Deng Hanxin, Chen Siyu, Meng Zihan, He Mengyao, Tu Ding, Wang He, Li Xian, Wang Fangyu, Lei Hexu, Yang Shifeng, Dong Huan, Xia Qingyou, Li Xueming, Wang Feng

机构信息

Integrative Science Center of Germplasm Creation in Western China (CHONGQING) Science City, Biological Science Research Center, Southwest University, Chongqing 400715, PR China.

Key Laboratory of Birth Defects and Related Diseases of Women and Children of Ministry of Education, Department of Radiology, West China Second University Hospital, Sichuan University, 20# South Renmin Road, Chengdu, Sichuan, PR China.

出版信息

Acta Biomater. 2025 Aug;202:216-233. doi: 10.1016/j.actbio.2025.07.030. Epub 2025 Jul 12.

Abstract

Ulcerative colitis (UC) is one type of inflammatory bowel diseases, and adiponectin (APN) is a potential therapeutic protein drug for treating UC. However, source and targeted delivery of APN to improve its effectiveness and bioavailability remain challenges. Here, we report a strategy to develop a sericin hydrogel (rhAPN-sh) through genetically engineering silkworm to spin silks mixed with recombinant human adiponectin (rhAPN), which efficiently overcome APN source and delivery. The rhAPN-sh exhibits desirable material performances such as stable internal crystal structure, fast swelling behavior, good biocompatibility, injectability. The rhAPN-sh effectively protected the APN through harsh gastroenteric environment for oral administration, which alleviated UC symptoms in mice with significant therapeutic effect by reconstructing colonic cell structure and colon length, reducing release of inflammatory factors, and maintaining stability of intestinal microbial population. These results indicate that the fabricated rhAPN-sh is a promising system for colitis treatment. STATEMENT OF SIGNIFICANCE: The present study presents an efficient strategy to treat ulcerative colitis (UC) by developing a genetically engineered sericin hydrogel delivering recombinant human adiponectin (rhAPN). Using transgenic silkworms, the system enables efficient rhAPN production, while the sericin hydrogel protects APN from gastrointestinal degradation, ensuring effective oral delivery. The sericin hydrogel alleviates UC symptoms in mice by reducing inflammation, restoring colon structure, and maintaining gut microbiota stability. This approach overcomes key challenges in APN protein drug delivery, offering a scalable, biocompatible, and effective therapeutic platform for UC and potentially other inflammatory diseases.

摘要

溃疡性结肠炎(UC)是炎症性肠病的一种类型,脂联素(APN)是一种治疗UC的潜在治疗性蛋白质药物。然而,APN的来源和靶向递送以提高其有效性和生物利用度仍然是挑战。在此,我们报告了一种通过基因工程蚕吐丝与重组人脂联素(rhAPN)混合来开发丝胶蛋白水凝胶(rhAPN-sh)的策略,该策略有效克服了APN的来源和递送问题。rhAPN-sh表现出理想的材料性能,如稳定的内部晶体结构、快速溶胀行为、良好的生物相容性、可注射性。rhAPN-sh通过口服给药在恶劣的胃肠环境中有效保护APN,通过重建结肠细胞结构和结肠长度、减少炎症因子释放以及维持肠道微生物群的稳定性,减轻了小鼠的UC症状,具有显著的治疗效果。这些结果表明,制备的rhAPN-sh是一种有前景的结肠炎治疗系统。重要性声明:本研究提出了一种通过开发递送重组人脂联素(rhAPN)的基因工程丝胶蛋白水凝胶来治疗溃疡性结肠炎(UC)的有效策略。利用转基因蚕,该系统能够高效生产rhAPN,同时丝胶蛋白水凝胶保护APN不被胃肠道降解,确保有效的口服递送。丝胶蛋白水凝胶通过减轻炎症、恢复结肠结构和维持肠道微生物群稳定性来减轻小鼠的UC症状。这种方法克服了APN蛋白质药物递送中的关键挑战,为UC以及潜在的其他炎症性疾病提供了一个可扩展、生物相容且有效的治疗平台。

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