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胶原亲和肽修饰的去细胞真皮基质通过持续释放Histatin-1 介导的促进血管生成加速糖尿病创面愈合。

Acellular dermal matrix decorated with collagen-affinity peptide accelerate diabetic wound healing through sustained releasing Histatin-1 mediated promotion of angiogenesis.

机构信息

Department of Limbs (Foot and Hand) Microsurgery, Chenzhou No.1 people's hospital, Chenzhou, China.

Key Laboratory of Organ Injury, Aging and Regenerative Medicine of Hunan Province, Changsha, China; Hunan Engineering Research Center of Sports and Health, Changsha, China.

出版信息

Int J Pharm. 2022 Aug 25;624:122017. doi: 10.1016/j.ijpharm.2022.122017. Epub 2022 Jul 15.

DOI:10.1016/j.ijpharm.2022.122017
PMID:35839983
Abstract

Treating diabetic ulcers is a major challenge in clinical practice, persecuting millions of patients with diabetes and increasing the medical burden. Recombinant growth factor application can accelerate diabetic wound healing via angiogenesis. The local administration of recombinant growth factors has no robust clinical efficiency because of the degradation of append short duration of the molecules in the hostile inflammatoryenvironment.The present study focused on the pathophysiology of impaired neovascularization and growth factor short duration in the diabetic wound. We prepared a collagen-binding domain (CBD)-fused recombinant peptide (C-Histatin-1) that had both pro-angiogenesis capacity and collagen-affinity properties. Next, we created a biocompatible acellular dermal matrix (ADM) as a drug delivery carrier that featured collagen-richness, high porosity, and non-cytotoxicity. C-Histatin-1 was then tethered on ADM to obtain a sustained-release effect. Finally, a functional scaffold (C-Hst1/ADM) was developed. C-Hst1/ADM can sustain-release Histatin-1 to promote the adhesion, migration, and angiogenesisof vascular endothelial cells in vitro. Using a diabetic wound model, we showed that C-Hst1/ADM could significantly promote angiogenesis, reduce scar widths, and improve extracellular collagen accumulation. Therefore, the results of this study provide a foundation for the clinical application of C-Hst1/ADM covering scaffold in the treatment of diabetic wounds.

摘要

治疗糖尿病性溃疡是临床实践中的一大挑战,困扰着数以百万计的糖尿病患者,并增加了医疗负担。重组生长因子的应用可以通过血管生成加速糖尿病伤口愈合。由于在敌对的炎症环境中分子的半衰期短,局部给予重组生长因子的临床效果并不理想。本研究集中于糖尿病伤口中受损的新血管生成和生长因子半衰期的病理生理学。我们制备了一种具有促血管生成能力和胶原亲和力特性的胶原结合域(CBD)融合重组肽(C-组蛋白-1)。接下来,我们创建了一种生物相容性的去细胞真皮基质(ADM)作为药物输送载体,其特点是富含胶原、高孔隙率和非细胞毒性。然后将 C-组蛋白-1 连接到 ADM 上以获得持续释放效果。最后,开发了一种功能性支架(C-Hst1/ADM)。C-Hst1/ADM 可以持续释放组蛋白-1,以促进体外血管内皮细胞的黏附、迁移和血管生成。使用糖尿病性伤口模型,我们表明 C-Hst1/ADM 可以显著促进血管生成、减少疤痕宽度和改善细胞外胶原积累。因此,这项研究的结果为 C-Hst1/ADM 覆盖支架在治疗糖尿病性伤口中的临床应用提供了基础。

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