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在模拟根治性前列腺切除术损伤的大鼠模型中,通过组织特异性旁分泌机制递送人间充质脂肪来源干细胞可恢复多种泌尿系统功能障碍。

Delivery of human mesenchymal adipose-derived stem cells restores multiple urological dysfunctions in a rat model mimicking radical prostatectomy damages through tissue-specific paracrine mechanisms.

作者信息

Yiou René, Mahrouf-Yorgov Meriem, Trébeau Céline, Zanaty Marc, Lecointe Cécile, Souktani Richard, Zadigue Patricia, Figeac Florence, Rodriguez Anne-Marie

机构信息

INSERM U955 Team 12, Créteil, France.

Université Paris-Est Créteil, UMR_S955, UPEC, Créteil, France.

出版信息

Stem Cells. 2016 Feb;34(2):392-404. doi: 10.1002/stem.2226. Epub 2015 Oct 23.

DOI:10.1002/stem.2226
PMID:26439006
Abstract

Urinary incontinence (UI) and erectile dysfunction (ED) are the most common functional urological disorders and the main sequels of radical prostatectomy (RP) for prostate cancer. Mesenchymal stem cell (MSC) therapy holds promise for repairing tissue damage due to RP. Because animal studies accurately replicating post-RP clinical UI and ED are lacking, little is known about the mechanisms underlying the urological benefits of MSC in this setting. To determine whether and by which mechanisms MSC can repair damages to both striated urethral sphincter (SUS) and penis in the same animal, we delivered human multipotent adipose stem cells, used as MSC model, in an immunocompetent rat model replicating post-RP UI and ED. In this model, we demonstrated by using noninvasive methods in the same animal from day 7 to day 90 post-RP injury that MSC administration into both the SUS and the penis significantly improved urinary continence and erectile function. The regenerative effects of MSC therapy were not due to transdifferentiation and robust engraftment at injection sites. Rather, our results suggest that MSC benefits in both target organs may involve a paracrine process with not only soluble factor release by the MSC but also activation of the recipient's secretome. These two effects of MSC varied across target tissues and damaged-cell types. In conclusion, our work provides new insights into the regenerative properties of MSC and supports the ability of MSC from a single source to repair multiple types of damage, such as those seen after RP, in the same individual.

摘要

尿失禁(UI)和勃起功能障碍(ED)是最常见的功能性泌尿系统疾病,也是前列腺癌根治性前列腺切除术(RP)的主要后遗症。间充质干细胞(MSC)疗法有望修复RP所致的组织损伤。由于缺乏准确复制RP后临床UI和ED的动物研究,人们对MSC在这种情况下产生泌尿系统益处的潜在机制知之甚少。为了确定MSC是否以及通过何种机制能够修复同一动物的尿道横纹括约肌(SUS)和阴茎的损伤,我们在一种免疫健全的大鼠模型中注入人多能脂肪干细胞(用作MSC模型),该模型复制了RP后的UI和ED。在这个模型中,我们在RP损伤后第7天至第90天,通过在同一动物身上使用非侵入性方法证明,向SUS和阴茎内注入MSC可显著改善尿失禁和勃起功能。MSC治疗的再生效果并非由于转分化和在注射部位的大量植入。相反,我们的结果表明,MSC在两个靶器官中的益处可能涉及旁分泌过程,不仅包括MSC释放可溶性因子,还包括激活受体的分泌组。MSC的这两种作用在不同的靶组织和受损细胞类型中有所不同。总之,我们的工作为MSC的再生特性提供了新的见解,并支持单一来源的MSC修复同一个体多种类型损伤(如RP后所见损伤)的能力。

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