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利用弹性蛋白生物聚合物共递送生长因子和组织保护分子可加速糖尿病小鼠的伤口愈合。

Co-delivery of a growth factor and a tissue-protective molecule using elastin biopolymers accelerates wound healing in diabetic mice.

机构信息

Center for Engineering in Medicine, Massachusetts General Hospital, Harvard Medical School, Shriners Hospitals for Children, Boston, MA, USA.

Center for Engineering in Medicine, Massachusetts General Hospital, Harvard Medical School, Shriners Hospitals for Children, Boston, MA, USA.

出版信息

Biomaterials. 2017 Oct;141:149-160. doi: 10.1016/j.biomaterials.2017.06.043. Epub 2017 Jun 30.

DOI:10.1016/j.biomaterials.2017.06.043
PMID:28688286
Abstract

Growth factor therapy is a promising approach for chronic diabetic wounds, but strategies to efficiently and cost-effectively deliver active molecules to the highly proteolytic wound environment remain as major obstacles. Here, we re-engineered keratinocyte growth factor (KGF) and the cellular protective peptide ARA290 into a protein polymer suspension with the purpose of increasing their proteolytic resistance, thus their activity in vivo. KGF and ARA290 were fused with elastin-like peptide (ELP), a protein polymer derived from tropoelastin, that confers the ability to separate into a colloidal suspension of liquid-like coacervates. ELP fusion did not diminish peptides activities as demonstrated by ability of KGF-ELP to accelerate keratinocyte proliferation and migration, and ARA290-ELP to protect cells from apoptosis. We examined the healing effect of ARA290-ELP and KGF-ELP alone or in combination, in a full-thickness diabetic wound model. In this model, ARA290-ELP was found to accelerate healing, notably by increasing angiogenesis in the wound bed. We further showed that co-delivery of ARA290 and KGF, with the 1:4 KGF-ELP to ARA290-ELP ratio, was the most effective wound treatment with the fastest healing rate, the thicker granulation tissue and regenerated epidermis after 28 days. Overall, this study shows that ARA290-ELP and KGF-ELP constitute promising new therapeutics for treatment of chronic wounds.

摘要

生长因子治疗是治疗慢性糖尿病创面的一种很有前途的方法,但如何有效地、经济高效地将活性分子递送到高度蛋白水解的创面环境仍然是主要障碍。在这里,我们将角质细胞生长因子 (KGF) 和细胞保护肽 ARA290 重新设计成一种蛋白聚合物悬浮液,目的是增加它们的蛋白水解抗性,从而提高它们在体内的活性。KGF 和 ARA290 与弹性蛋白样肽 (ELP) 融合,ELP 是一种源自原弹性蛋白的蛋白聚合物,具有分离成类似胶体的凝聚物胶态悬浮液的能力。ELP 融合并没有降低肽的活性,这可以从 KGF-ELP 加速角质细胞增殖和迁移的能力以及 ARA290-ELP 保护细胞免受凋亡的能力中得到证明。我们在全层糖尿病创面模型中单独或联合检测了 ARA290-ELP 和 KGF-ELP 的愈合效果。在该模型中,发现 ARA290-ELP 可加速愈合,特别是通过增加创面床中的血管生成。我们进一步表明,以 1:4 的 KGF-ELP 与 ARA290-ELP 比例共递送 ARA290 和 KGF 是最有效的创面治疗方法,其愈合速度最快,28 天后的肉芽组织和再生表皮最厚。总的来说,这项研究表明 ARA290-ELP 和 KGF-ELP 构成了治疗慢性创面的有前途的新疗法。

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