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源自诱导多能干细胞的无基质人肺类器官用于模拟肺损伤。

Matrix-free human lung organoids derived from induced pluripotent stem cells to model lung injury.

作者信息

Budeus Bettina, Kroepel Chiara, Stasch Lisa Marie, Klein Diana

机构信息

Institute for Cell Biology (Cancer Research), University Hospital Essen, University of Duisburg-Essen, Essen, Germany.

出版信息

Stem Cell Res Ther. 2024 Dec 18;15(1):468. doi: 10.1186/s13287-024-04106-3.

Abstract

BACKGROUND

Organoids, as near-physiological 3D culture systems, offer new opportunities to study the pathogenesis of various organs in mimicking the cellular complexity and functionality of human organs.

METHOD

Here we used a quite simple and very practicable method to successfully generate induced pluripotent stem cell (iPSC)-derived human lung organoids (LuOrg) in a matrix-free manner as an alternative to the widely used preclinical mouse models in order to investigate normal lung damage in detail and as close as possible to the patient. We performed detailed morphological and molecular analyses, including bulk and single cell RNA sequencing, of generated lung organoids and evaluated the quality and robustness of our model as a potential in vitro platform for lung diseases, namely radiation-induced lung injury.

RESULTS

A matrix-free method for differentiation of iPSCs can be used to obtain lung organoids that morphologically reflect the target tissue of the human lung very well, especially with regard to the cellular composition. The different cellular fates were investigated following the genotoxic stress induced by radiation and revealed further insights in the radiation-sensitivity of the different lung cells. Finally, we provide cellular gene sets found to be induced in the different lung organoid cellular subsets after irradiation, which could be used as additional RT response and particularly senescence gene sets in future studies.

CONCLUSION

By establishing these free-floating LuOrgs for the investigation of cancer therapeutic approaches as a new and patient-oriented in vitro platform particularly in experimental radiooncology, not only a reduction in the number of experimental animals, but also an adequately and meaningfully replacement of corresponding animal experiments can be achieved.

摘要

背景

类器官作为接近生理状态的三维培养系统,为研究各种器官的发病机制提供了新机会,可模拟人体器官的细胞复杂性和功能。

方法

在此,我们采用一种非常简单且切实可行的方法,以无基质方式成功生成诱导多能干细胞(iPSC)来源的人肺类器官(LuOrg),作为广泛使用的临床前小鼠模型的替代方案,以便详细研究正常肺损伤并尽可能贴近患者情况。我们对生成的肺类器官进行了详细的形态学和分子分析,包括大量和单细胞RNA测序,并评估了我们的模型作为肺部疾病(即放射性肺损伤)潜在体外平台的质量和稳健性。

结果

一种用于iPSC分化的无基质方法可用于获得在形态上能很好反映人肺靶组织的肺类器官,尤其是在细胞组成方面。在辐射诱导的基因毒性应激后研究了不同的细胞命运,并揭示了不同肺细胞对辐射敏感性的更多见解。最后,我们提供了照射后在不同肺类器官细胞亚群中发现的诱导细胞基因集,这些基因集可在未来研究中用作额外的放疗反应特别是衰老基因集。

结论

通过建立这些用于研究癌症治疗方法的自由漂浮LuOrg,作为一个新的、以患者为导向的体外平台,特别是在实验放射肿瘤学中,不仅可以减少实验动物的数量,还可以充分且有意义地替代相应的动物实验。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/a822/11657174/0ba725c18066/13287_2024_4106_Fig1_HTML.jpg

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