SFI CÚRAM Centre for Research in Medical Devices, National University of Ireland Galway, Galway City, Ireland.
School of Physics, and National University of Ireland Galway, Galway City, Ireland.
Tissue Eng Part C Methods. 2021 Feb;27(2):77-88. doi: 10.1089/ten.TEC.2020.0331.
Bioengineering of skin has been significantly explored, ranging from the use of traditional cell culture systems to the most recent organ-on-a-chip (OoC) technology that permits skin modeling on physiological scales among other benefits. This article presents key considerations for developing physiologically relevant immunocompetent diabetic foot ulcer (DFU) models. Diabetic foot ulceration affects hundreds of millions of individuals globally, especially the elderly, and constitutes a major socioeconomic burden. When DFUs are not treated and managed in a timely manner, 15-50% of patients tend to undergo partial or complete amputation of the affected limb. Consequently, at least 40% of such patients die within 5 years postamputation. Currently, therapeutic strategies are actively sought and developed. However, present-day preclinical platforms (animals and models) are not robust enough to provide reliable data for clinical trials. Insights from published works on immunocompetent skin-on-a-chip models and bioengineering considerations, presented in this article, can inform researchers on how to develop robust OoC models for testing topical therapies such as growth factor-based therapies for DFUs. We propose that immunocompetent DFU-on-a-chip models should be bioengineered using diseased cells derived from individuals; in particular, the pathophysiological contribution of macrophages in diabetic wound healing, along with the typical fibroblasts and keratinocytes, needs to be recapitulated. The ideal model should consist of the following components: diseased cells embedded in reproducible scaffolds, which permit endogenous "diseased" extracellular matrix deposition, and the integration of the derived immunocompetent DFU model onto a microfluidic platform. The proposed DFU platforms will eventually facilitate reliable and robust drug testing of wound healing therapeutics, coupled with reduced clinical trial failure rates. Impact statement Current animal and cell-based systems are not physiologically relevant enough to retrieve reliable results for clinical translation of diabetic foot ulcer (DFU) therapies. Organ-on-a-chip (OoC) technology offers desirable features that could finally enable the vision of modeling DFU for pathophysiological studies and drug testing at a microscale. This article brings together the significant recent findings relevant to developing a minimally functional immunocompetent DFU-on-a-chip model, as wound healing cannot occur without a proper functioning immune response. It looks feasible in the future to recapitulate the stagnant inflammation in DFU (thought to impede wound healing) using OoC, diseased cells, and an endogenously produced extracellular matrix.
皮肤的生物工程已经得到了广泛的探索,从传统的细胞培养系统到最近的器官芯片(OoC)技术,这些技术都可以在生理尺度上模拟皮肤,具有其他优势。本文介绍了开发具有生理相关性的免疫活性糖尿病足溃疡(DFU)模型的关键注意事项。糖尿病足溃疡影响着全球数亿人,尤其是老年人,这给社会经济带来了巨大的负担。如果不及时治疗和管理 DFU,15-50%的患者可能会出现受影响肢体的部分或完全截肢。因此,至少有 40%的此类患者在截肢后 5 年内死亡。目前,正在积极寻求和开发治疗方法。然而,目前的临床前平台(动物和模型)还不够强大,无法为临床试验提供可靠的数据。本文介绍了发表的关于免疫活性皮肤芯片模型和生物工程的见解,可以为研究人员提供信息,帮助他们开发用于测试局部治疗的稳健的 OoC 模型,如基于生长因子的 DFU 治疗。我们建议使用源自个体的患病细胞来生物工程免疫活性 DFU 芯片模型;特别是,需要重现巨噬细胞在糖尿病伤口愈合中的病理生理贡献,以及典型的成纤维细胞和角质形成细胞。理想的模型应包括以下组成部分:患病细胞嵌入可重复的支架中,允许内源性“患病”细胞外基质的沉积,并将衍生的免疫活性 DFU 模型集成到微流控平台上。所提出的 DFU 平台最终将有助于可靠和稳健的伤口愈合治疗药物的测试,同时降低临床试验失败率。 影响声明 目前的动物和基于细胞的系统还不够生理相关,无法为糖尿病足溃疡(DFU)治疗的临床转化提供可靠的结果。器官芯片(OoC)技术具有理想的特点,最终可以实现对 DFU 进行病理生理学研究和药物测试的微观建模。本文汇集了与开发最小功能免疫活性 DFU 芯片模型相关的重要最新发现,因为没有适当的免疫反应,伤口愈合就无法进行。在未来,使用 OoC、患病细胞和内源性产生的细胞外基质来重现 DFU 中的停滞性炎症(被认为会阻碍伤口愈合)似乎是可行的。
