Mario Negri Institute for Pharmacological Research, Centro Anna Maria Astori, Science and Technology Park Kilometro Rosso, Bergamo, Italy.
Stem Cells Dev. 2013 Mar 1;22(5):772-80. doi: 10.1089/scd.2012.0266. Epub 2012 Dec 21.
Bone marrow-mesenchymal stem cells (BM-MSC) ameliorate renal dysfunction and repair tubular damage of acute kidney injury by locally releasing growth factors, including the insulin-like growth factor-1 (IGF-1). The restricted homing of BM-MSC at the site of injury led us to investigate a possible gene-based communication mechanism between BM-MSC and tubular cells. Human BM-MSC (hBM-MSC) released microparticles and exosomes (Exo) enriched in mRNAs. A selected pattern of transcripts was detected in Exo versus parental cells. Exo expressed the IGF-1 receptor (IGF-1R), but not IGF-1 mRNA, while hBM-MSC contained both mRNAs. R- cells lacking IGF-1R exposed to hBM-MSC-derived Exo acquired the human IGF-1R transcript that was translated in the corresponding protein. Transfer of IGF-1R mRNA from Exo to cisplatin-damaged proximal tubular cells (proximal tubular epithelial cell [PTEC]) increased PTEC proliferation. Coincubation of damaged PTEC with Exo and soluble IGF-1 further enhanced cell proliferation. These findings suggest that horizontal transfer of the mRNA for IGF-1R to tubular cells through Exo potentiates tubular cell sensitivity to locally produced IGF-1 providing a new mechanism underlying the powerful renoprotection of few BM-MSC observed in vivo.
骨髓间充质干细胞(BM-MSC)通过局部释放生长因子,包括胰岛素样生长因子-1(IGF-1),改善肾功能并修复急性肾损伤的肾小管损伤。BM-MSC 在损伤部位的归巢受限,这促使我们研究 BM-MSC 与肾小管细胞之间可能存在基因通讯机制。人 BM-MSC(hBM-MSC)释放富含 mRNAs 的微泡和外泌体(Exo)。与亲本细胞相比,在外泌体中检测到了特定的转录本模式。外泌体表达 IGF-1 受体(IGF-1R),但不表达 IGF-1 mRNA,而 hBM-MSC 则同时含有这两种 mRNA。暴露于 hBM-MSC 衍生的外泌体的缺乏 IGF-1R 的 R-细胞获得了人 IGF-1R 转录本,该转录本被翻译成相应的蛋白质。从外泌体向顺铂损伤的近端肾小管细胞(近端肾小管上皮细胞 [PTEC])转移 IGF-1R mRNA 增加了 PTEC 的增殖。将受损的 PTEC 与外泌体和可溶性 IGF-1 共孵育进一步增强了细胞增殖。这些发现表明,通过外泌体将 IGF-1R 的 mRNA 横向转移到肾小管细胞中,增加了肾小管细胞对局部产生的 IGF-1 的敏感性,为体内观察到的少数 BM-MSC 具有强大的肾保护作用提供了一种新的机制。
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