首页> 美国卫生研究院文献>Marine Drugs >Bioactive Glial-Derived Neurotrophic Factor from a Safe Injectable Collagen–Alginate Composite Gel Rescues Retinal Photoreceptors from Retinal Degeneration in Rabbits
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Bioactive Glial-Derived Neurotrophic Factor from a Safe Injectable Collagen–Alginate Composite Gel Rescues Retinal Photoreceptors from Retinal Degeneration in Rabbits

机译:来自安全注射胶原蛋白-海藻酸盐复合凝胶的生物活性神经胶质衍生神经营养因子可拯救兔子视网膜光感受器免受视网膜变性

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摘要

The management of vision-threatening retinal diseases remains challenging due to the lack of an effective drug delivery system. Encapsulated cell therapy (ECT) offers a promising approach for the continuous delivery of therapeutic agents without the need for immunosuppressants. In this context, an injectable and terminable collagen–alginate composite (CAC) ECT gel, designed with a Tet-on pro-caspase-8 system, was developed as a safe intraocular drug delivery platform for the sustained release of glial-cell-line-derived neurotrophic factor (GDNF) to treat retinal degenerative diseases. This study examined the potential clinical application of the CAC ECT gel, focusing on its safety, performance, and termination through doxycycline (Dox) administration in the eyes of healthy New Zealand White rabbits, as well as its therapeutic efficacy in rabbits with sodium-iodate (SI)-induced retinal degeneration. The findings indicated that the CAC ECT gel can be safely implanted without harming the retina or lens, displaying resistance to degradation, facilitating cell attachment, and secreting bioactive GDNF. Furthermore, the GDNF levels could be modulated by the number of implants. Moreover, Dox administration was effective in terminating gel function without causing retinal damage. Notably, rabbits with retinal degeneration treated with the gels exhibited significant functional recovery in both a-wave and b-wave amplitudes and showed remarkable efficacy in reducing photoreceptor apoptosis. Given its biocompatibility, mechanical stability, controlled drug release, terminability, and therapeutic effectiveness, our CAC ECT gel presents a promising therapeutic strategy for various retinal diseases in a clinical setting, eliminating the need for immunosuppressants.
机译:由于缺乏有效的药物输送系统,威胁视力的视网膜疾病的管理仍然具有挑战性。包埋细胞疗法 (ECT) 提供了一种很有前途的方法,无需免疫抑制剂即可连续递送治疗药物。在这种情况下,开发了一种可注射和可终止的胶原蛋白-海藻酸盐复合 (CAC) ECT 凝胶,其设计有 Tet-on pro-caspase-8 系统,作为一种安全的眼内药物递送平台,用于持续释放神经胶质细胞系衍生的神经营养因子 (GDNF) 以治疗视网膜退行性疾病。本研究考察了 CAC ECT 凝胶的潜在临床应用,重点关注其安全性、性能和通过多西环素 (Dox) 给药在健康新西兰白兔眼中的终止,以及其对碘酸钠 (SI) 诱导的视网膜变性的兔子的治疗效果。研究结果表明,CAC ECT 凝胶可以安全地植入,而不会伤害视网膜或晶状体、表现出抗降解性、促进细胞粘附和分泌生物活性 GDNF。此外,GDNF 水平可以通过植入物的数量来调节。此外,Dox 给药可有效终止凝胶功能而不会造成视网膜损伤。值得注意的是,用凝胶处理的视网膜变性兔子在 a 波和 b 波振幅上都表现出显着的功能恢复,并且在减少光感受器凋亡方面显示出显着的疗效。鉴于其生物相容性、机械稳定性、药物释放控制、终止性和治疗效果,我们的 CAC ECT 凝胶在临床环境中为各种视网膜疾病提供了一种有前途的治疗策略,无需免疫抑制剂。

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