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经黏膜移植的间充质干细胞通过促进血管生成来刺激肠道愈合。

Mucosally transplanted mesenchymal stem cells stimulate intestinal healing by promoting angiogenesis.

作者信息

Manieri Nicholas A, Mack Madison R, Himmelrich Molly D, Worthley Daniel L, Hanson Elaine M, Eckmann Lars, Wang Timothy C, Stappenbeck Thaddeus S

出版信息

J Clin Invest. 2015 Sep;125(9):3606-18. doi: 10.1172/JCI81423. Epub 2015 Aug 17.

Abstract

Mesenchymal stem cell (MSC) therapy is an emerging field of regenerative medicine; however, it is often unclear how these cells mediate repair. Here, we investigated the use of MSCs in the treatment of intestinal disease and modeled abnormal repair by creating focal wounds in the colonic mucosa of prostaglandin-deficient mice. These wounds developed into ulcers that infiltrated the outer intestinal wall. We determined that penetrating ulcer formation in this model resulted from increased hypoxia and smooth muscle wall necrosis. Prostaglandin I₂ (PGI₂) stimulated VEGF-dependent angiogenesis to prevent penetrating ulcers. Treatment of mucosally injured WT mice with a VEGFR inhibitor resulted in the development of penetrating ulcers, further demonstrating that VEGF is critical for mucosal repair. We next used this model to address the role of transplanted colonic MSCs (cMSCs) in intestinal repair. Compared with intravenously injected cMSCs, mucosally injected cMSCs more effectively prevented the development of penetrating ulcers, as they were more efficiently recruited to colonic wounds. Importantly, mucosally injected cMSCs stimulated angiogenesis in a VEGF-dependent manner. Together, our results reveal that penetrating ulcer formation results from a reduction of local angiogenesis and targeted injection of MSCs can optimize transplantation therapy. Moreover, local MSC injection has potential for treating diseases with features of abnormal angiogenesis and repair.

摘要

间充质干细胞(MSC)疗法是再生医学中一个新兴的领域;然而,这些细胞如何介导修复作用往往并不明确。在此,我们研究了间充质干细胞在肠道疾病治疗中的应用,并通过在前列腺素缺乏小鼠的结肠黏膜上制造局灶性伤口来模拟异常修复过程。这些伤口发展成溃疡,并浸润到肠壁外层。我们确定,该模型中穿透性溃疡的形成是由于缺氧增加和平滑肌壁坏死所致。前列腺素I₂(PGI₂)刺激依赖血管内皮生长因子(VEGF)的血管生成,从而预防穿透性溃疡。用VEGFR抑制剂治疗黏膜损伤的野生型小鼠会导致穿透性溃疡的形成,这进一步证明VEGF对黏膜修复至关重要。接下来,我们利用这个模型来探讨移植的结肠间充质干细胞(cMSC)在肠道修复中的作用。与静脉注射的cMSC相比,黏膜注射的cMSC能更有效地预防穿透性溃疡的形成,因为它们能更有效地被募集到结肠伤口处。重要的是,黏膜注射的cMSC以依赖VEGF的方式刺激血管生成。总之,我们的研究结果表明,穿透性溃疡的形成是由于局部血管生成减少所致,而靶向注射间充质干细胞可以优化移植治疗。此外,局部注射间充质干细胞对于治疗具有异常血管生成和修复特征的疾病具有潜在价值。

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