用富含地塞米松-微孔板的生物相容性胶原- PDMS生物支架加强胰岛移植

ty10086 提交于 周三, 08/25/2021 - 16:18
文章英文标题
Enhancing islet transplantation using a biocompatible collagen-PDMS bioscaffold enriched with dexamethasone-microplates
正文
胰岛移植是使1型糖尿病患者独立于胰岛素注射而获得血糖控制的一种很有前景的方法。然而,高达60 %的胰岛在移植后立即丢失。为了改善这一结果,胰岛可以在生物支架内移植,然而人工合成的生物支架会引起强烈的炎症反应,对胰岛功能和存活有不利影响。在本研究中,我们首先通过胶原包复聚二甲基硅氧烷( PDMS )生物支架来改善其生物相容性。为减少对PDMS生物支架的炎症反应,我们随后用地塞米松负载的微板( DEX-μScaffolds )富集生物支架。这些DEX-微板具有在不影响胰岛葡萄糖反应性但可使周围微环境炎症最小化的治疗范围内持续7周以上释放DEX的能力。该生物支架具有优良的力学性能,能够抵抗孔隙塌陷,从而有助于胰岛的种植和植入,并在附睾脂肪垫( EFP )内进行移植手术。使用DEX-μScaffolds将胰岛移植到糖尿病小鼠的EFP内后,第4天基础血糖恢复到正常值,天。此外,这些动物对葡萄糖挑战表现出正常的动态反应,组织学证据显示移植部位DEX-μScaffolds周围促炎细胞因子和纤维组织减少。相比之下,在胰岛功能整体较差的基础条件下,单纯移植胰岛或不移植DEX微板的生物支架内胰岛的糖尿病动物均不能恢复血糖控制。综合考虑,我们的数据显示,用胶原包被PDMS生物支架,并用DEX-微孔板富集,显著延长和增强胰岛功能和存活。
文章内容(英文)
Islet transplantation is a promising approach to enable type 1 diabetic patients to attain glycemic control independent of insulin injections. However, up to 60% of islets are lost immediately following transplantation. To improve this outcome, islets can be transplanted within bioscaffolds, however, synthetic bioscaffolds induce an intense inflammatory reaction which can have detrimental effects on islet function and survival. In the present study, we first improved the biocompatibility of polydimethylsiloxane (PDMS) bioscaffolds by coating them with collagen. To reduce the inflammatory response to PDMS bioscaffolds, we then enriched the bioscaffolds with dexamethasone-loaded microplates (DEX-μScaffolds). These DEX-microplates have the ability to release DEX in a sustained manner over 7 weeks within a therapeutic range that does not affect the glucose responsiveness of the islets but which minimizes inflammation in the surrounding microenvironment. The bioscaffold showed excellent mechanical properties that enabled it to resist pore collapse thereby helping to facilitate islet seeding and its handling for implantation, and subsequent engraftment, within the epididymal fat pad (EFP). Following the transplantation of islets into the EFP of diabetic mice using DEX-μScaffolds there was a return in basal blood glucose to normal values by day 4, with normoglycemia maintained for 30 d. Furthermore, these animals demonstrated a normal dynamic response to glucose challenges with histological evidence showing reduced pro-inflammatory cytokines and fibrotic tissue surrounding DEX-μScaffolds at the transplantation site. In contrast, diabetic animals transplanted with either islets alone or islets in bioscaffolds without DEX microplates were not able to regain glycemic control during basal conditions with overall poor islet function. Taken together, our data show that coating PDMS bioscaffolds with collagen, and enriching them with DEX-microplates, significantly prolongs and enhances islet function and survival.
来源出处
Journal|[J]BiofabricationVolume 13, Issue 3. 2021.
DOI
https://doi.org/10.1088/1758-5090/ABDCAC

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