Engineering and Monitoring the Sustained Release of Extracellular Vesicles from Hydrogels for In Vivo Therapeutic Applications

IF 4 Q2 ENGINEERING, BIOMEDICAL
Selen Uman, Noah Weingarten, Mark Helmers, Amit Iyengar, Karen L. Xu, Kendra Worthington, Danika Meldrum, Jessica Dominic, Sara Guevara-Plunkett, Alexis Schiazza, Pavan Atluri, Jason A. Burdick
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Abstract

Extracellular vesicles (EVs) are gaining interest in regenerative medicine and biomaterials have been shown to extend EV bioavailability following delivery. Herein, the labeling of both hydrogels and EVs is reported to better understand hydrogel design for sustained EV release into tissues. Shear-thinning hydrogels are engineered using guest–host (i.e., adamantane–cyclodextrin) modifications to hyaluronic acid (GH), as well as GH hydrogels with the addition of gelatin crosslinked via transglutaminase (GH+Gel) to temporally control hydrogel properties. When labeled with a near-IR dye and injected into rat myocardial tissue, the GH+Gel hydrogel is retained (>14 days) longer than the GH hydrogel alone (≈7 days), likely due to the added gelatin network. To overcome challenges associated with common EV labeling methods, a highly versatile metabolic labeling methodology is utilized via the incorporation of N-azidoacetylmannosamine-tetraacylated during EV synthesis to introduce azide groups that can then be reacted with DBCO dyes. When injected in saline, EVs are cleared within 24 h in hearts; however, hydrogels enhance EV retention, with levels based on hydrogel degradation behavior, namely, >14 days for GH+Gel hydrogel and ≈7 days for GH hydrogel alone. These findings support the use of hydrogels in EV therapies.

Abstract Image

为体内治疗应用设计并监测水凝胶中细胞外囊泡的持续释放
细胞外囊泡(EVs)在再生医学中越来越受到关注,生物材料已被证明可在递送后延长 EVs 的生物利用度。本文报告了水凝胶和EVs的标记情况,以更好地了解水凝胶的设计,从而将EVs持续释放到组织中。利用客体-宿主(即金刚烷-环糊精)对透明质酸(GH)进行修饰,设计出了剪切稀化水凝胶,以及添加了通过转谷氨酰胺酶交联的明胶(GH+Gel)的GH水凝胶,以在时间上控制水凝胶的特性。当用近红外染料标记并注射到大鼠心肌组织中时,GH+Gel 水凝胶比单独的 GH 水凝胶保留的时间(14 天)更长(≈7 天),这可能是由于添加了明胶网络。为了克服与常见 EV 标记方法相关的挑战,我们采用了一种高度通用的代谢标记方法,即在 EV 合成过程中加入 N-叠氮乙酰甘露聚糖四乙酰化,以引入叠氮基团,然后与 DBCO 染料反应。在生理盐水中注射时,EV 会在心脏中 24 小时内清除;然而,水凝胶会增强 EV 的保留,根据水凝胶的降解行为,GH+Gel 水凝胶可保留 14 天,而单独使用 GH 水凝胶则可保留≈7 天。这些发现支持在 EV 治疗中使用水凝胶。
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来源期刊
Advanced Nanobiomed Research
Advanced Nanobiomed Research nanomedicine, bioengineering and biomaterials-
CiteScore
5.00
自引率
5.90%
发文量
87
审稿时长
21 weeks
期刊介绍: Advanced NanoBiomed Research will provide an Open Access home for cutting-edge nanomedicine, bioengineering and biomaterials research aimed at improving human health. The journal will capture a broad spectrum of research from increasingly multi- and interdisciplinary fields of the traditional areas of biomedicine, bioengineering and health-related materials science as well as precision and personalized medicine, drug delivery, and artificial intelligence-driven health science. The scope of Advanced NanoBiomed Research will cover the following key subject areas: ▪ Nanomedicine and nanotechnology, with applications in drug and gene delivery, diagnostics, theranostics, photothermal and photodynamic therapy and multimodal imaging. ▪ Biomaterials, including hydrogels, 2D materials, biopolymers, composites, biodegradable materials, biohybrids and biomimetics (such as artificial cells, exosomes and extracellular vesicles), as well as all organic and inorganic materials for biomedical applications. ▪ Biointerfaces, such as anti-microbial surfaces and coatings, as well as interfaces for cellular engineering, immunoengineering and 3D cell culture. ▪ Biofabrication including (bio)inks and technologies, towards generation of functional tissues and organs. ▪ Tissue engineering and regenerative medicine, including scaffolds and scaffold-free approaches, for bone, ligament, muscle, skin, neural, cardiac tissue engineering and tissue vascularization. ▪ Devices for healthcare applications, disease modelling and treatment, such as diagnostics, lab-on-a-chip, organs-on-a-chip, bioMEMS, bioelectronics, wearables, actuators, soft robotics, and intelligent drug delivery systems. with a strong focus on applications of these fields, from bench-to-bedside, for treatment of all diseases and disorders, such as infectious, autoimmune, cardiovascular and metabolic diseases, neurological disorders and cancer; including pharmacology and toxicology studies.
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