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P 物质通过调节间充质干细胞的血管生成潜能增强其治疗效果。

Substance P enhances the therapeutic effect of MSCs by modulating their angiogenic potential.

机构信息

Department of Biomedical Science and Technology, Graduate School, Kyung Hee University, Seoul, Korea.

East-West Medical Research Institute, Kyung Hee University Hospital, Seoul, Korea.

出版信息

J Cell Mol Med. 2020 Nov;24(21):12560-12571. doi: 10.1111/jcmm.15804. Epub 2020 Sep 28.

Abstract

Bone marrow mesenchymal stem cell (MSC) therapy acts through multiple differentiations in damaged tissue or via secretion of paracrine factors, as demonstrated in various inflammatory and ischaemic diseases. However, long-term ex vivo culture to obtain a sufficient number of cells in MSC transplantation leads to cellular senescence, deficiency of the paracrine potential, and loss of survival rate post-transplantation. In this study, we evaluated whether supplementation of MSCs with substance P (SP) can improve their therapeutic potential. SP treatment elevated the secretion of paracrine/angiogenic factors, including VEGF, SDF-1a and PDGF-BB, from late passage MSCs in vitro. MSCs supplemented with SP accelerated epidermal/dermal regeneration and neovascularization and suppressed inflammation in vivo, compared to MSCs transplanted alone. Importantly, supplementation with SP enabled the incorporation of transplanted human MSCs into the host vasculature as pericytes via PDGF signalling, leading to the direct engagement of transplanted cells in compact vasculature formation. Our results showed that SP is capable of restoring the cellular potential of senescent stem cells, possibly by modulating the generation of paracrine factors from MSCs, which might accelerate MSC-mediated tissue repair. Thus, SP is anticipated to be a potential beneficial agent in MSC therapy for inflammatory or ischaemic diseases and cutaneous wounds.

摘要

骨髓间充质干细胞(MSC)治疗通过在受损组织中的多种分化或通过旁分泌因子的分泌起作用,如在各种炎症和缺血性疾病中所证明的那样。然而,为了在 MSC 移植中获得足够数量的细胞,长期的体外培养会导致细胞衰老、旁分泌潜能不足和移植后存活率降低。在这项研究中,我们评估了用 P 物质(SP)补充 MSC 是否可以提高其治疗潜力。SP 处理可提高体外晚期传代 MSC 旁分泌/血管生成因子(包括 VEGF、SDF-1a 和 PDGF-BB)的分泌。与单独移植 MSC 相比,SP 补充的 MSC 可加速表皮/真皮再生和新血管生成,并抑制体内炎症。重要的是,SP 的补充使移植的人 MSC 通过 PDGF 信号转导整合到宿主血管中作为周细胞,从而使移植细胞直接参与致密血管形成。我们的结果表明,SP 能够恢复衰老干细胞的细胞潜能,可能通过调节 MSC 旁分泌因子的产生,从而加速 MSC 介导的组织修复。因此,SP 有望成为炎症或缺血性疾病和皮肤创伤中 MSC 治疗的潜在有益剂。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/fb4f/7687016/57edb3123de9/JCMM-24-12560-g001.jpg

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