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Endometrial stem cells repair injured endometrium and induce angiogenesis via AKT and ERK pathways

机译:子宫内膜干细胞通过AKT和ERK通路修复受损的子宫内膜并诱导血管生成

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Intrauterine adhesions are common acquired endometrial syndromes secondary to endometrial injury, with limited effective therapies. Recently, several studies have reported that bone marrow stem cells (BMSCs) could repair injured endometrium in animal experiments. However, the role of stem cells in endometrial injury repair and its therapeutic mechanisms remain unclear. Here, we established mouse endometrial injury model and examined the benefit of human endometrial mesenchymal stem cells derived from menstrual blood (MenSCs) in restoration of injured endometrium. Injured endometrium exhibited significantly accelerated restoration at Day 7 after MenSCs transplantation, with increased endometrial thickness and microvessel density. Moreover, the fertility of mice with injured endometrium was improved, with higher conception rate (53.57% vs 14.29%, P?=?0.014) and larger embryo number (3.1?±?0.6 vs 0.9?±?0.7, P?=?0.030) in MenSCs group than control group, while no difference was found in undamaged horns between two groups. Conditioned medium from MenSCs (MenSCs-CM) could decrease H2O2-induced apoptosis of human umbilical vein endothelial cells (HUVECs) and promote proliferation, migration and angiogenesis. Angiogenesis effect of MenSCs-CM was also confirmed in Matrigel plug assay in mice. Furthermore, we discovered that MenSCs-CM could activate AKT and ERK pathways and induce the overexpression of eNOS, VEGFA, VEGFR1, VEGFR2 and TIE2 in HUVECs, which are critical in MenSCs-CM-induced angiogenesis. Angiogenesis induced by MenSCs-CM could be reversed by inhibitors of AKT and/or ERK. Taken together, we concluded that MenSCs could restore injured endometrium and improve the fertility of the endometrial injury mice, which was partially attributed to angiogenesis induced by MenSCs.
机译:宫腔粘连是继发于子宫内膜损伤的常见获得性子宫内膜综合征,有效疗法有限。最近,一些研究报道了骨髓干细胞(BMSC)可以在动物实验中修复受损的子宫内膜。然而,干细胞在子宫内膜损伤修复中的作用及其治疗机制仍不清楚。在这里,我们建立了小鼠子宫内膜损伤模型,并研究了来自月经血(MenSCs)的人子宫内膜间充质干细胞在受损子宫内膜恢复中的益处。 MenSCs移植后第7天,受伤的子宫内膜显示出明显加速的恢复,子宫内膜厚度和微血管密度增加。此外,子宫内膜损伤的小鼠的受精能力得到改善,受胎率更高(53.57%对14.29%,P <= 0.014)和更大的胚胎数(3.1±±0.6 vs 0.9 +±0.7,P = 0.05)。 MenSCs组比对照组低0.030),而两组未受损的角没有发现差异。 MenSCs的条件培养基(MenSCs-CM)可以减少H2O2诱导的人脐静脉内皮细胞(HUVECs)凋亡,并促进增殖,迁移和血管生成。 MenSCs-CM的血管生成作用也已在小鼠的Matrigel塞栓试验中得到证实。此外,我们发现MenSCs-CM可以激活AKT和ERK通路,并诱导HUVEC中eNOS,VEGFA,VEGFR1,VEGFR2和TIE2的过表达,这在MenSCs-CM诱导的血管生成中至关重要。 MenSCs-CM诱导的血管生成可以被AKT和/或ERK抑制剂逆转。综上所述,我们得出的结论是MenSCs可以恢复受损的子宫内膜并改善子宫内膜损伤小鼠的生育能力,这部分归因于MenSCs诱导的血管生成。

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