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通过水解激活、产氧的生物材料预防β细胞和胰岛中的缺氧诱导的细胞死亡。

Preventing hypoxia-induced cell death in beta cells and islets via hydrolytically activated, oxygen-generating biomaterials.

机构信息

Diabetes Research Institute and Departments of Surgery and Medicine, Leonard M. Miller School of Medicine, University of Miami, Miami, FL 33136, USA.

出版信息

Proc Natl Acad Sci U S A. 2012 Mar 13;109(11):4245-50. doi: 10.1073/pnas.1113560109. Epub 2012 Feb 27.

Abstract

A major hindrance in engineering tissues containing highly metabolically active cells is the insufficient oxygenation of these implants, which results in dying or dysfunctional cells in portions of the graft. The development of methods to increase oxygen availability within tissue-engineered implants, particularly during the early engraftment period, would serve to allay hypoxia-induced cell death. Herein, we designed and developed a hydrolytically activated oxygen-generating biomaterial in the form of polydimethylsiloxane (PDMS)-encapsulated solid calcium peroxide, PDMS-CaO(2). Encapsulation of solid peroxide within hydrophobic PDMS resulted in sustained oxygen generation, whereby a single disk generated oxygen for more than 6 wk at an average rate of 0.026 mM per day. The ability of this oxygen-generating material to support cell survival was evaluated using a β cell line and pancreatic rat islets. The presence of a single PDMS-CaO(2) disk eliminated hypoxia-induced cell dysfunction and death for both cell types, resulting in metabolic function and glucose-dependent insulin secretion comparable to that in normoxic controls. A single PDMS-CaO(2) disk also sustained enhanced β cell proliferation for more than 3 wk under hypoxic culture conditions. Incorporation of these materials within 3D constructs illustrated the benefits of these materials to prevent the development of detrimental oxygen gradients within large implants. Mathematical simulations permitted accurate prediction of oxygen gradients within 3D constructs and highlighted conditions under which supplementation of oxygen tension would serve to benefit cellular viability. Given the generality of this platform, the translation of these materials to other cell-based implants, as well as ischemic tissues in general, is envisioned.

摘要

在工程组织中含有高度代谢活跃的细胞时,一个主要的障碍是这些植入物的氧合不足,这导致移植物的部分细胞死亡或功能失调。开发增加组织工程植入物中氧气可用性的方法,特别是在早期植入期间,将有助于减轻缺氧诱导的细胞死亡。在此,我们设计并开发了一种水解激活的氧气生成生物材料,其形式为聚二甲基硅氧烷(PDMS)封装的固体过氧化钙,PDMS-CaO(2)。将固体过氧化物封装在疏水性 PDMS 内导致持续的氧气生成,其中一个圆盘在平均每天 0.026mM 的速率下产生氧气超过 6 周。使用β细胞系和胰岛大鼠评估了这种产氧材料支持细胞存活的能力。单个 PDMS-CaO(2)圆盘的存在消除了两种细胞类型的缺氧诱导的细胞功能障碍和死亡,导致代谢功能和葡萄糖依赖性胰岛素分泌与正常氧合对照组相当。单个 PDMS-CaO(2)圆盘还在缺氧培养条件下维持增强的β细胞增殖超过 3 周。将这些材料纳入 3D 构建体中说明了这些材料的益处,以防止在大植入物中形成有害的氧气梯度。数学模拟允许准确预测 3D 构建体中的氧气梯度,并突出了补充氧气张力将有益于细胞活力的条件。鉴于这个平台的普遍性,预计这些材料将被转化为其他基于细胞的植入物,以及一般的缺血组织。

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