释放动力学对局部递送甲状旁腺激素骨再生应用效果的影响。

Tissue Engineering Part A Pub Date : 2021-02-01 Epub Date: 2020-09-10 DOI:10.1089/ten.TEA.2020.0119
Samantha J Wojda, Ian A Marozas, Kristi S Anseth, Michael J Yaszemski, Seth W Donahue
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引用次数: 2

摘要

表征材料定向局部递送生物活性分子的释放特征及其对骨再生的影响是提高我们对骨愈合反应的理解和优化能力的重要一步。本研究使用嵌入多孔聚富马酸丙烯(PPF)支架的巯基水凝胶检测甲状旁腺激素(PTH)的局部递送,用于骨再生应用。本研究的目的是表征巯基水凝胶中PTH的体外降解控制释放动力学,皮下植入模型中的体内水凝胶降解以及大鼠临界大小骨缺损的骨愈合。将甲状旁腺激素捆绑在水凝胶基质上,消除了在先前的体外研究中观察到的甲状旁腺激素自由扩散出基质的早期时间点爆发释放。在最初的2周内,只有8%的PTH从水凝胶中释放出来,但到第21天,80%的PTH被释放,到第28天完全释放。体内植入显示,水凝胶在第21天完全降解;然而,当将水凝胶掺入三维打印的骨导电性PPF支架中时,水凝胶的持续时间>56天。研究发现,使用复合巯基水凝胶- ppf支架治疗骨缺损时,给予3或10 μg的栓系PTH 1-84,可增加临界大小骨缺损的桥接,而使用30 μg的栓系PTH治疗可减少骨长入缺损区域。这种用于甲状旁腺激素的生物材料递送系统的持续发展可能会导致治疗骨不连骨折和临界大小骨缺损的方法的改进。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
Impact of Release Kinetics on Efficacy of Locally Delivered Parathyroid Hormone for Bone Regeneration Applications.

Characterizing the release profile for materials-directed local delivery of bioactive molecules and its effect on bone regeneration is an important step to improve our understanding of, and ability to optimize, the bone healing response. This study examined the local delivery of parathyroid hormone (PTH) using a thiol-ene hydrogel embedded in a porous poly(propylene fumarate) (PPF) scaffold for bone regeneration applications. The aim of this study was to characterize the degradation-controlled in vitro release kinetics of PTH from the thiol-ene hydrogels, in vivo hydrogel degradation in a subcutaneous implant model, and bone healing in a rat critical size bone defect. Tethering PTH to the hydrogel matrix eliminated the early timepoint burst release that was observed in previous in vitro work where PTH was free to diffuse out of the matrix. Only 8% of the tethered PTH was released from the hydrogel during the first 2 weeks, but by day 21, 80% of the PTH was released, and complete release was achieved by day 28. In vivo implantation revealed that complete degradation of the hydrogel alone occurred by day 21; however, when incorporated in a three-dimensional printed osteoconductive PPF scaffold, the hydrogel persisted for >56 days. Treatment of bone defects with the composite thiol-ene hydrogel-PPF scaffold, delivering either 3 or 10 μg of tethered PTH 1-84, was found to increase bridging of critical size bone defects, whereas treatment with 30 μg of tethered PTH resulted in less bone ingrowth into the defect area. Continued development of this biomaterial delivery system for PTH could lead to improved therapies for treatment of nonunion fractures and critical size bone defects.

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Tissue Engineering Part A
Tissue Engineering Part A CELL & TISSUE ENGINEERING-BIOTECHNOLOGY & APPLIED MICROBIOLOGY
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