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羊膜干细胞来源的促血管生成可溶性因子在缺血性筋膜皮瓣模型中募集内皮祖细胞。

Proangiogenic soluble factors from amniotic fluid stem cells mediate the recruitment of endothelial progenitors in a model of ischemic fasciocutaneous flap.

机构信息

Department of Experimental Medicine-DIMES, University of Genova, Genova, Italy.

出版信息

Stem Cells Dev. 2012 Aug 10;21(12):2179-88. doi: 10.1089/scd.2011.0639. Epub 2012 Mar 6.

DOI:10.1089/scd.2011.0639
PMID:22225409
Abstract

Skin flaps are routinely used in surgery for the functional and cosmetic repair of wounds or disfiguring scars. The recent concept of therapeutic angiogenesis has emerged as an attractive approach to overcome the problem of blood supply deficiency, often resulting in the flap grafting failure. In the present study, we embedded a gelatin membrane with amniotic fluid stem cells (AFSC) derived conditioned media (ACM) to topically deliver angiogenic growth factors and cytokines into a rat model of ischemic full-thickness skin flap elevated in the epigastric region. AFSC secretome triggered the endogenous repair by the recruitment of endothelial progenitor cells. We studied the vascular perfusion rate, the vessel distribution, and the survival of ACM-treated flaps. In detail, the ischemic sectors of ACM-treated flaps showed at day 7 a perfusion level 50% higher than the preoperation baseline. The ensuing necrosis development was delayed and the histology analysis showed a normal arrangement of epidermal and dermal structures and a high density of vessels in subcutaneous tissues. Further, we found that ACM recruited CD31⁺/VEGFR2⁺ and CD31⁺/CD34⁺ cells into the ischemic subcutaneous tissues and that the isolated progenitors were capable to form clusters of von Willebrand factor-positive cells in culture. We propose ACM as a cell-free cocktail of chemokines and growth factors to be adopted for clinical applications.

摘要

皮瓣在外科手术中常用于功能和美容修复伤口或畸形疤痕。最近出现的治疗性血管生成概念是一种有吸引力的方法,可以克服血液供应不足的问题,这通常会导致皮瓣移植失败。在本研究中,我们将含有羊水干细胞(AFSC)来源条件培养基(ACM)的明胶膜用于局部递送血管生成生长因子和细胞因子到大鼠模型中,在该模型中,腹部皮瓣被提升以模拟缺血性全层皮肤瓣。AFSC 分泌组通过募集内皮祖细胞触发内源性修复。我们研究了血管灌注率、血管分布和 ACM 处理皮瓣的存活率。具体来说,在第 7 天,ACM 处理的皮瓣缺血区域的灌注水平比术前基线高 50%。随后的坏死发展被延迟,组织学分析显示表皮和真皮结构的正常排列以及皮下组织中高血管密度。此外,我们发现 ACM 将 CD31⁺/VEGFR2⁺和 CD31⁺/CD34⁺细胞募集到缺血的皮下组织中,并且分离的祖细胞能够在培养中形成 von Willebrand 因子阳性细胞的簇。我们提出 ACM 作为一种无细胞的趋化因子和生长因子鸡尾酒,可用于临床应用。

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