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在临床前环境中设计并评估一种用于急性肝衰竭的 3D 打印可植入药物输送装置的设计和可用性。

Design and Usability Evaluations of a 3D-Printed Implantable Drug Delivery Device for Acute Liver Failure in Preclinical Settings.

机构信息

Department of Biotechnology, The Catholic University of Korea, 43 Jibong-ro, Bucheon-Si, Gyeonggi-do, 14662, Republic of Korea.

Department of Biomedical-Chemical Engineering, The Catholic University of Korea, 43 Jibong-ro, Bucheon-Si, Gyeonggi-do, 14662, Republic of Korea.

出版信息

Adv Healthc Mater. 2021 Jul;10(14):e2100497. doi: 10.1002/adhm.202100497. Epub 2021 Jun 23.

Abstract

Acute liver failure (ALF) requiring liver transplantation is a disease that occurs due to rapid hepatocellular dysfunction. As liver transplantation has various limitations, including donor scarcity, high cost, and immuno-incompatibility, continuous local delivery of biopharmaceuticals to the liver tissue can be a promising ALF treatment option. Here, the in vivo safety and usability of a 3D-printed implantable drug delivery device for effective ALF treatment is evaluated. The implantable reservoir consists of a 3D-printed container and a semipermeable membrane for repeated administrations of drugs, specifically to the liver tissue. The physical stability and function of the 3D-printed reservoir are confirmed by the mechanical properties and in vitro drug release test, respectively. In mice implanted with the reservoir system, mortality, weight changes, clinical signs, hematological and serum biochemical changes, and organ weight changes are not observed, suggesting no foreign body reaction. The usability of the reservoir system is further evaluated using an ALF model of 70% hepatectomized mice treated with N-acetylcysteine through the system, showing cell-specific regeneration and significant liver injury alleviation. Overall, the 3D-printed reservoir system is safe for studying the therapeutic potential of ALF treatment, and it can be used for the delivery of various active pharmaceutical ingredients.

摘要

急性肝衰竭(ALF)需要进行肝移植,这种疾病是由于肝细胞快速功能障碍引起的。由于肝移植存在各种限制,包括供体短缺、成本高和免疫相容性等问题,因此持续将生物制药局部递送到肝组织可能是一种有前途的 ALF 治疗选择。本研究评估了一种 3D 打印可植入药物输送装置用于有效治疗 ALF 的体内安全性和可用性。该可植入储库由 3D 打印容器和半渗透膜组成,可重复给药,特别是递送到肝组织。通过机械性能和体外药物释放试验分别确认了 3D 打印储库的物理稳定性和功能。在植入储库系统的小鼠中,未观察到死亡率、体重变化、临床症状、血液学和血清生化变化以及器官重量变化,表明没有异物反应。进一步通过系统用 N-乙酰半胱氨酸治疗 70%肝切除的 ALF 模型评估了储库系统的可用性,结果显示细胞特异性再生和显著减轻肝损伤。总的来说,3D 打印储库系统可安全地用于研究 ALF 治疗的治疗潜力,并且可用于输送各种活性药物成分。

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