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间充质干细胞条件培养基在肠道类器官系统中的辐射反应及再生效应评估

Evaluation of the radiation response and regenerative effects of mesenchymal stem cell-conditioned medium in an intestinal organoid system.

作者信息

Kim Young-Heon, Han Sung-Hoon, Kim Hyewon, Lee Sun-Joo, Joo Hyun-Woo, Kim Min-Jung, Shim Sehwan, Kim Kyuchang, Lee Janet, Jang Won-Suk, Park Sunhoo, Jang Hyosun, Lee Seung Bum

机构信息

Laboratory of Radiation Exposure and Therapeutics, National Radiation Emergency Medical Center, Korea Institute of Radiological and Medical Science, Seoul, Republic of Korea.

出版信息

Biotechnol Bioeng. 2020 Dec;117(12):3639-3650. doi: 10.1002/bit.27543. Epub 2020 Sep 11.

DOI:10.1002/bit.27543
PMID:32833232
Abstract

Intestinal organoids have recently emerged as an in vitro model relevant to the gut system owing to their recapitulation of the native intestinal epithelium with crypt-villus architecture. However, it is unclear whether intestinal organoids reflect the physiology of the in vivo stress response. Here, we systemically investigated the radiation response in organoids and animal models using mesenchymal stem cell-conditioned medium (MSC-CM), which contains secreted paracrine factors. Irradiated organoids exhibited sequential induction of viability loss and regrowth after irradiation (within 12 days), similar to the response of the native intestinal epithelium. Notably, treatment with MSC-CM facilitated the reproliferation of intestinal stem cells (ISCs) and restoration of damaged crypt-villus structures in both models. Furthermore, Wnt/Notch signaling pathways were commonly upregulated by MSC-CM, but not radiation, and pharmacologically selective inhibition of Wnt or Notch signaling attenuated the enhanced recovery of irradiated organoids, with increases in ISCs, following MSC-CM treatment. Interestingly, the expression of Wnt4, Wnt7a, and active β-catenin was increased, but not notch family members, in MSC-CM-treated organoid after irradiation. Treatment of recombinant mouse Wnt4 and Wnt7a after irradiation improved to some extent intestinal epithelial regeneration both in vitro and in vivo. Overall, these results suggested that intestinal organoids recapitulated the physiological stress response of the intestinal epithelium in vivo. Thus, our findings provided important insights into the physiology of intestinal organoids and may contribute to the development of strategies to enhance the functional maturation of engineered organoids.

摘要

由于肠类器官能够重现具有隐窝 - 绒毛结构的天然肠上皮,最近它已成为一种与肠道系统相关的体外模型。然而,尚不清楚肠类器官是否反映了体内应激反应的生理学特征。在这里,我们使用含有分泌性旁分泌因子的间充质干细胞条件培养基(MSC-CM),系统地研究了类器官和动物模型中的辐射反应。照射后的类器官在照射后(12天内)表现出活力丧失和再生的顺序诱导,类似于天然肠上皮的反应。值得注意的是,在两个模型中,用MSC-CM处理都促进了肠干细胞(ISC)的再增殖以及受损隐窝 - 绒毛结构的恢复。此外,Wnt/Notch信号通路通常被MSC-CM上调,但不受辐射上调,并且对Wnt或Notch信号的药理学选择性抑制减弱了照射后类器官在MSC-CM处理后ISC增加的增强恢复。有趣的是,在照射后的MSC-CM处理的类器官中,Wnt4、Wnt7a和活性β-连环蛋白的表达增加,但Notch家族成员的表达没有增加。照射后用重组小鼠Wnt4和Wnt7a处理在体外和体内都在一定程度上改善了肠上皮再生。总体而言,这些结果表明肠类器官重现了体内肠上皮的生理应激反应。因此,我们的发现为肠类器官的生理学提供了重要见解,并可能有助于制定增强工程化类器官功能成熟的策略。

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