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Augmentation of Dermal Wound Healing by Adipose Tissue-Derived Stromal Cells (ASC)

机译:脂肪组织基质细胞(ASC)增强皮肤伤口愈合

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摘要

The skin is the largest organ of the human body and is the first line of defense against physical and biological damage. Thus, the skin is equipped to self-repair and regenerates after trauma. Skin regeneration after damage comprises a tightly spatial-temporally regulated process of wound healing that involves virtually all cell types in the skin. Wound healing features five partially overlapping stages: homeostasis, inflammation, proliferation, re-epithelization, and finally resolution or fibrosis. Dysreguled wound healing may resolve in dermal scarring. Adipose tissue is long known for its suppressive influence on dermal scarring. Cultured adipose tissue-derived stromal cells (ASCs) secrete a plethora of regenerative growth factors and immune mediators that influence processes during wound healing e.g., angiogenesis, modulation of inflammation and extracellular matrix remodeling. In clinical practice, ASCs are usually administered as part of fractionated adipose tissue i.e., as part of enzymatically isolated SVF (cellular SVF), mechanically isolated SVF (tissue SVF), or as lipograft. Enzymatic isolation of SVF obtained adipose tissue results in suspension of adipocyte-free cells (cSVF) that lack intact intercellular adhesions or connections to extracellular matrix (ECM). Mechanical isolation of SVF from adipose tissue destructs the parenchyma (adipocytes), which results in a tissue SVF (tSVF) with intact connections between cells, as well as matrix. To date, due to a lack of well-designed prospective randomized clinical trials, neither cSVF, tSVF, whole adipose tissue, or cultured ASCs can be indicated as the preferred preparation procedure prior to therapeutic administration. In this review, we present and discuss current literature regarding the different administration options to apply ASCs (i.e., cultured ASCs, cSVF, tSVF, and lipografting) to augment dermal wound healing, as well as the available indications for clinical efficacy.
机译:皮肤是人体最大的器官,是抵御物理和生物损害的第一道防线。因此,皮肤能够自我修复并在创伤后再生。损伤后的皮肤再生包括伤口愈合的严格时空调节过程,实际上涉及皮肤中的所有细胞类型。伤口愈合具有五个部分重叠的阶段:稳态,炎症,增殖,再上皮化,最后是消融或纤维化。伤口愈合不良可以解决皮肤瘢痕形成。众所周知,脂肪组织对皮肤瘢痕形成有抑制作用。培养的源自脂肪组织的基质细胞(ASC)分泌过多的再生生长因子和免疫介质,这些因子会影响伤口愈合过程中的过程,例如血管生成,炎症调节和细胞外基质重塑。在临床实践中,ASC通常作为分级脂肪组织的一部分,即作为酶分离的SVF(细胞SVF),机械分离的SVF(组织SVF)或脂质移植的一部分给药。酶法分离获得的SVF脂肪组织会导致无脂肪细胞悬浮细胞(cSVF)悬浮,该细胞缺乏完整的细胞间粘附或与细胞外基质(ECM)的连接。从脂肪组织机械分离SVF破坏了实质(脂肪细胞),这导致组织SVF(tSVF)在细胞和基质之间具有完整的连接。迄今为止,由于缺乏精心设计的前瞻性随机临床试验,在治疗性给药之前,不能将cSVF,tSVF,整个脂肪组织或培养的ASCs指示为优选的制备方法。在这篇综述中,我们介绍和讨论有关应用ASC(即培养的ASC,cSVF,tSVF和脂质移植)以增加皮肤伤口愈合的不同给药方式的现有文献,以及有关临床疗效的可用指征。

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