Stem Cell Therapy Unit, Jesús Usón Minimally Invasive Surgery Centre, 10071, Cáceres, Spain.
RICORS-TERAV Network, ISCIII, 28029, Madrid, Spain.
Mol Med. 2023 Apr 4;29(1):48. doi: 10.1186/s10020-023-00646-1.
Despite constant advances in regenerative medicine, the closure of chronic wounds is still challenging. Therapeutic approaches using locally administered MSCs have been considered a promising option. However, the viability of these cells is seriously threatened by acute hypoxic stress linked to wound healing. In this work, we aimed to study the tolerance of Menstrual blood-derived stromal cells (MenSCs) to acute hypoxia and their therapeutic paracrine effect.
Isolated MenSCs were phenotypically characterized and evaluated in terms of proliferation, viability, and gene expression, under acute hypoxia (AH) compared with conventional cultured condition or normoxia (N). A step further, the secretome of MenSCs under acute hypoxia was analyzed with respect to their miRNAs content and by in vitro functional assays. For the analysis of differences between the two groups, Student's t-test was performed and one-way ANOVA and Tukey's multiple comparisons test for multiple groups were used.
Our results revealed that the viability of MenSCs was not affected under acute hypoxia, although proliferation rate slowed down. Gene analysis revealed 5 up-regulated (BNIP3, ANGPTL4, IL6, IL1B, and PDK1) and 4 down-regulated genes (IDO1, HMOX1, ANGPTL2, and HGF) in AH compared to N. Global gene expression analysis revealed a decrease in the gene ontology functions of migration and wound response with respect to the normoxic condition. In contrast, functions such as angiogenesis were enriched under the AH condition. Regarding the secretome analysis, two miRNAs involved in angiogenic processes (hsa-miR-148a-3p and hsa-miR-378a-3p), were significantly up-expressed when compared to the normoxic condition, being MYC gene, the unique target of both. Functional assays on HUVECs revealed a potential pro-angiogenic capacity of MenSCs cultured in both oxygen conditions (N and AH) based on the wound closure and tube formation results of their released paracrine factors. However, when compared to normoxia, the paracrine factors of MenSCs under acute hypoxia slightly reduced the proliferation, migration, and in vitro wound closure of HUVECs.
MenSC exhibited a good survival capacity under acute hypoxic conditions as well as beneficial properties applicable in the field of tissue regeneration through their secretome, which makes them a potential cell source for wound healing interventions.
尽管再生医学不断取得进展,但慢性伤口的闭合仍然具有挑战性。局部应用间充质干细胞的治疗方法被认为是一种很有前途的选择。然而,这些细胞的活力受到与伤口愈合相关的急性低氧应激的严重威胁。在这项工作中,我们旨在研究月经血源性基质细胞(MenSCs)对急性缺氧的耐受性及其治疗性旁分泌作用。
分离的 MenSCs 进行表型鉴定,并在急性低氧(AH)与常规培养条件或常氧(N)下进行增殖、活力和基因表达评估。进一步,分析 MenSCs 在急性低氧下的分泌组,分析其 miRNA 含量和体外功能。为了分析两组之间的差异,进行了学生 t 检验,对于多组进行了单因素方差分析和 Tukey 多重比较检验。
我们的结果表明,MenSCs 的活力在急性低氧下不受影响,尽管增殖速度减慢。基因分析显示,与 N 相比,AH 中有 5 个上调基因(BNIP3、ANGPTL4、IL6、IL1B 和 PDK1)和 4 个下调基因(IDO1、HMOX1、ANGPTL2 和 HGF)。全基因表达分析显示,与常氧条件相比,迁移和伤口反应的基因本体功能减少。相反,血管生成等功能在 AH 条件下富集。关于分泌组分析,两个参与血管生成过程的 miRNA(hsa-miR-148a-3p 和 hsa-miR-378a-3p)与常氧条件相比显著上调,其唯一靶基因是 MYC。基于其释放的旁分泌因子的伤口闭合和管形成结果,在两种氧气条件(N 和 AH)下培养的 MenSCs 对 HUVECs 具有潜在的促血管生成能力。然而,与常氧相比,急性低氧下 MenSCs 的旁分泌因子略微降低了 HUVECs 的增殖、迁移和体外伤口闭合。
MenSC 在急性低氧条件下具有良好的生存能力,并通过其分泌组具有适用于组织再生领域的有益特性,使其成为伤口愈合干预的潜在细胞来源。
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