矿化成骨细胞衍生的外泌体let-7f-5p通过DUSP1/Erk1/2信号通路促进内皮细胞血管生成

IF 3.1 3区 生物学 Q2 BIOTECHNOLOGY & APPLIED MICROBIOLOGY Journal of Tissue Engineering and Regenerative Medicine Pub Date : 2022-11-08 DOI:10.1002/term.3358
Yiqun He, Hailong Li, Zuochong Yu, Linli Li, Xujun Chen, Aolei Yang, Feizhou Lyu, Youhai Dong
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引用次数: 0

摘要

血管的形成是组织工程骨存活和生长的先决条件。矿化成骨细胞(MOBs)已被证明通过分泌含有各种促血管生成因子的外泌体来调节血管生成。然而,含有let-7f-5p的矿化成骨细胞衍生外泌体(mobo - exos)是否能调节内皮细胞(ECs)的血管生成尚不清楚。本研究通过体外和体内研究,比较了分别用mobo - exos、let-7f-5p模拟mobo - exos (miR模拟组)和let-7f-5p抑制mobo - exos (miR抑制剂组)处理的ECs的血管生成能力。此外,通过验证Erk1/2信号通路和靶基因DUSP1的作用,探讨了mobo - exo let-7f-5p调控血管生成的潜在机制。结果表明,mobo - exos能显著促进内皮细胞血管生成,模拟外泌体let-7f-5p能增强内皮细胞血管生成,抑制外泌体let-7f-5p能减弱内皮细胞血管生成。Let-7f-5p可以抑制宽型DUSP1的荧光素酶活性,而DUSP1的突变可以取消Let-7f-5p的抑制能力。DUSP1的表达趋势与pErk1/2的表达趋势相反。与mobo - exos组相比,miR mimic组的pErk1/2表达明显升高,miR抑制剂组的pErk1/2表达明显降低,而抑制pErk1/2可部分损害内皮细胞的血管生成能力。综上所述,我们认为来源于MOBs的外泌体let-7f-5p可以通过激活DUSP1/Erk1/2信号通路促进ECs血管生成,这可能是促进组织工程骨血管生成的一个有希望的靶点。
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Exosomal let-7f-5p derived from mineralized osteoblasts promotes the angiogenesis of endothelial cells via the DUSP1/Erk1/2 signaling pathway

Blood vessel formation is the prerequisite for the survival and growth of tissue-engineered bone. Mineralized osteoblasts (MOBs) have been shown to regulate angiogenesis through the secretion of exosomes containing various pro-angiogenic factors. However, whether the mineralized osteoblast-derived exosomes (MOB-Exos) containing let-7f-5p can regulate the angiogenesis of endothelial cells (ECs) is still unknown. In this study, the angiogenic capabilities of ECs respectively treated with MOB-Exos, let-7f-5p mimicked MOB-Exos (miR mimic group), and let-7f-5p inhibited MOB-Exos (miR inhibitor group) were compared through in vitro and in vivo studies. Moreover, the potential mechanism of MOB-Exo let-7f-5p regulating angiogenesis was explored by verifying the role of the Erk1/2 signaling pathway and target gene DUSP1. The results showed that MOB-Exos could significantly promote the angiogenesis of ECs, which could be enhanced by mimicked exosomal let-7f-5p and attenuated by inhibited exosomal let-7f-5p. Let-7f-5p could suppress the luciferase activity of wide-type DUSP1, and the mutation of DUSP1 could abrogate the repressive ability of let-7f-5p. Furthermore, the expression of DUSP1 exhibited a reversed trend to that of pErk1/2. The expression of pErk1/2 was significantly higher in the miR mimic group and lower in the miR inhibitor group than that in the MOB-Exos group, while inhibition of pErk1/2 could partly impair the angiogenic capabilities of ECs. In conclusion, we concluded that exosomal let-7f-5p derived from MOBs could promote the angiogenesis of ECs via activating the DUSP1/Erk1/2 signaling pathway, which might be a promising target for promoting the angiogenesis of tissue-engineered bone.

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来源期刊
CiteScore
7.50
自引率
3.00%
发文量
97
审稿时长
4-8 weeks
期刊介绍: Journal of Tissue Engineering and Regenerative Medicine publishes rapidly and rigorously peer-reviewed research papers, reviews, clinical case reports, perspectives, and short communications on topics relevant to the development of therapeutic approaches which combine stem or progenitor cells, biomaterials and scaffolds, growth factors and other bioactive agents, and their respective constructs. All papers should deal with research that has a direct or potential impact on the development of novel clinical approaches for the regeneration or repair of tissues and organs. The journal is multidisciplinary, covering the combination of the principles of life sciences and engineering in efforts to advance medicine and clinical strategies. The journal focuses on the use of cells, materials, and biochemical/mechanical factors in the development of biological functional substitutes that restore, maintain, or improve tissue or organ function. The journal publishes research on any tissue or organ and covers all key aspects of the field, including the development of new biomaterials and processing of scaffolds; the use of different types of cells (mainly stem and progenitor cells) and their culture in specific bioreactors; studies in relevant animal models; and clinical trials in human patients performed under strict regulatory and ethical frameworks. Manuscripts describing the use of advanced methods for the characterization of engineered tissues are also of special interest to the journal readership.
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