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Functional Performance of Human Cardiosphere-derived Cells Delivered in an In Situ Polymerizable Hyaluronan-Gelatin Hydrogel

机译:在原位聚合透明质酸盐 - 明胶水凝胶中递送人体心脏源衍生细胞的功能性能

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摘要

The vast majority of cells delivered into the heart by conventional means are lost within the first 24 hours. Methods are needed to enhance cell retention, so as to minimize loss of precious material and maximize effectiveness of the therapy. We tested a cell-hydrogel delivery strategy. Cardiosphere-derived cells (CDCs) were grown from adult human cardiac biopsy specimens. In situ polymerizable hydrogels made of hyaluronan and porcine gelatin (Hystem®-C™) were formulated as a liquid at room temperature so as to gel within 20 minutes at 37°C. CDC viability and migration were not compromised in Hystem-C™. Myocardial infarction was created in SCID mice and CDCs were injected intramyocardially in the infarct border zone. Real time PCR revealed engraftment of CDCs delivered in Hystem-C™ was increased by nearly an order of magnitude. LVEF (left ventricular ejection fraction) deteriorated in the control (PBS only) group over the 3-week time course. Hystem-C™ alone or CDCs alone preserved LVEF relative to baseline, while CDCs delivered in Hystem-C™ resulted in a sizable boost in LVEF. Heart morphometry revealed the greatest attenuation of LV remodeling in the CDC + Hystem-C™ group. Histological analysis suggested cardiovascular differentiation of the CDCs in Hystem-C™. However, the majority of functional benefit is likely from paracrine mechanisms such as tissue preservation and neovascularization. A CDC/hydrogel formulation suitable for catheter-based intramyocardial injection exhibits superior engraftment and functional benefits relative to naked CDCs.
机译:通过常规手段递送到心脏中的绝大多数细胞在前24小时内丧失。需要增强细胞保留的方法,以尽量减少珍贵物质的损失并最大限度地提高治疗的有效性。我们测试了一种细胞 - 水凝胶输送策略。基石衍生的细胞(CDC)从成年人体心脏活检标本生长。在由透明质酸和猪明胶(Hysem®-C™)制成的原位聚合肼水凝胶在室温下配制成液体,以在37℃下在20分钟内凝胶。 CDC活力和迁移在Hystem-C™中没有损害。在SCID小鼠中产生心肌梗死,CDC在梗死边界区肌内内注射。实时PCR揭示了在函数-C™中递送的CDC的植入增加了几个数量级。 LVEF(左心室射血分数)在3周时间课程中对照(仅限PBS仅)劣化。单独的Hystem-C™独自保存LVEF相对于基线,而在Hystem-C™中提供的CDC导致LVEF升高。心灵形状学揭示了CDC +型CDC +型CD™组中LV重塑的最大衰减。组织学分析表明卫生系统-C™中CDC的心血管分化。然而,大多数功能性益处可能来自帕拉克碱机制,例如组织保存和新血管形成。适用于基于导管的肌动脉内注射的CDC /水凝胶制剂具有相对于裸CDC的卓越的植入和功能性益处。

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