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注射用胶原蛋白生物材料治疗心肌梗死的相关益处与时机有关。

Timing underpins the benefits associated with injectable collagen biomaterial therapy for the treatment of myocardial infarction.

机构信息

Division of Cardiac Surgery, University of Ottawa Heart Institute, Ottawa K1Y 4W7, Canada; Department of Cellular and Molecular Medicine, University of Ottawa, Ottawa K1H 8M5, Canada.

Division of Cardiac Surgery, University of Ottawa Heart Institute, Ottawa K1Y 4W7, Canada.

出版信息

Biomaterials. 2015 Jan;39:182-92. doi: 10.1016/j.biomaterials.2014.11.004. Epub 2014 Nov 22.

Abstract

Injectable hydrogel biomaterials are promising therapies to promote repair and regeneration post-myocardial infarction (MI). However, the timing of delivery and the mechanisms through which biomaterial treatments confer their benefits are translational issues that remain to be addressed. We assessed the efficacy of an injectable collagen matrix at 3 different delivery time points post-MI. Infarcted mice received the matrix or control (saline) treatment at 3 h, 1 week or 2 weeks after MI. The earlier treatment delivery better prevented negative ventricular remodeling and long-term deterioration of cardiac function (up to 3 months), whereas waiting longer to administer the matrix (1 and 2 weeks post-MI) reduced the therapeutic effects. Collagen matrix delivery did not stimulate an inflammatory response acutely and favorably modulated inflammation in the myocardium long-term. We found that the matrix interacts with the host tissue to alter the myocardial cytokine profile, promote angiogenesis, and reduce fibrosis and cell death. This work highlights that the timing of delivery can significantly affect the ability of an injectable hydrogel to protect the post-MI environment, which will be an important consideration in the clinical translation of cardiac biomaterial therapy.

摘要

可注射水凝胶生物材料是一种很有前途的治疗方法,可以促进心肌梗死后的修复和再生。然而,生物材料治疗的输送时间和机制是转化问题,仍有待解决。我们评估了可注射胶原基质在心肌梗死后 3 个不同时间点的疗效。在心肌梗死后 3 小时、1 周或 2 周,梗死小鼠接受了基质或对照(生理盐水)治疗。更早的治疗输送更好地防止了负性心室重构和心脏功能的长期恶化(长达 3 个月),而等待更长时间给予基质(心肌梗死后 1 周和 2 周)则降低了治疗效果。胶原基质输送不会在急性时引起炎症反应,并在长期内对心肌炎症进行有利的调节。我们发现,基质与宿主组织相互作用,改变心肌细胞因子谱,促进血管生成,减少纤维化和细胞死亡。这项工作强调了输送时间可以显著影响可注射水凝胶保护心肌梗死后环境的能力,这将是心脏生物材料治疗临床转化的一个重要考虑因素。

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