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间充质干细胞治疗可刺激内源性宿主祖细胞,促进结肠上皮再生。

Mesenchymal stem cell therapy stimulates endogenous host progenitor cells to improve colonic epithelial regeneration.

机构信息

Laboratory of Radiopathology and Experimental Therapeutics, Institute for Radiological Protection and Nuclear Safety, Fontenay-aux-Roses, France.

出版信息

PLoS One. 2013 Jul 29;8(7):e70170. doi: 10.1371/journal.pone.0070170. Print 2013.

Abstract

Patients who undergo pelvic radiotherapy may develop severe and chronic complications resulting from gastrointestinal alterations. The lack of curative treatment highlights the importance of novel and effective therapeutic strategies. We thus tested the therapeutic benefit of mesenchymal stem cells (MSC) treatment and proposed molecular mechanisms of action. MSC efficacy was tested in an experimental model of radiation-induced severe colonic ulceration histologically similar to that observed in patients. In this model, MSC from bone marrow were administered intravenously, immediately or three weeks (established lesions) after irradiation. MSC therapy reduces radiation-induced colonic ulceration and increases animal survival. MSC treatment induces therapeutic efficacy whatever the time of cell infusion. Infused-MSC engraft in the colon but also increase endogenous MSC mobilization in blood that have lasting benefits over time. In vitro analysis demonstrates that the MSC effect is mediated by paracrine mechanisms through the non-canonical WNT (Wingless integration site) pathway. In irradiated rat colons, MSC treatment increases the expression of the non-canonical WNT4 ligand by epithelial cells. The epithelial regenerative process is improved after MSC injection by stimulation of colonic epithelial cells positive for SOX9 (SRY-box containing gene 9) progenitor/stem cell markers. This study demonstrates that MSC treatment induces stimulation of endogenous host progenitor cells to improve the regenerative process and constitutes an initial approach to arguing in favor of the use of MSC to limit/reduce colorectal damage induced by radiation.

摘要

接受盆腔放射治疗的患者可能会因胃肠道改变而发生严重和慢性并发症。缺乏治愈性治疗方法突出了新型有效治疗策略的重要性。因此,我们测试了间充质干细胞(MSC)治疗的治疗效果,并提出了作用的分子机制。我们在一种与患者观察到的相似的辐射诱导严重结肠溃疡的实验模型中测试了 MSC 的疗效。在该模型中,骨髓来源的 MSC 通过静脉内给予,在照射后立即或 3 周(已建立的病变)给予。MSC 治疗可减少辐射诱导的结肠溃疡并提高动物存活率。无论细胞输注时间如何,MSC 治疗均可诱导治疗效果。输注的 MSC 定植在结肠中,并且还增加血液中内源性 MSC 的动员,随着时间的推移具有持久的益处。体外分析表明,MSC 效应是通过旁分泌机制通过非经典 WNT(Wingless 整合位点)途径介导的。在照射的大鼠结肠中,MSC 治疗通过刺激 SOX9(含 SRY 盒基因 9)祖细胞/干细胞标志物阳性的结肠上皮细胞增加上皮细胞中非经典 WNT4 配体的表达。这项研究表明,MSC 治疗可刺激内源性宿主祖细胞来改善再生过程,这构成了支持使用 MSC 来限制/减少辐射引起的结直肠损伤的初步方法。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/e9c7/3726425/fa534d514ab9/pone.0070170.g001.jpg

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