A tumorigenicity evaluation platform for cell therapies based on brain organoids.

IF 10.8 1区 医学 Q1 NEUROSCIENCES Translational Neurodegeneration Pub Date : 2024-10-29 DOI:10.1186/s40035-024-00446-5
Jun Xue, Youjun Chu, Yanwang Huang, Ming Chen, Meng Sun, Zhiqin Fan, Yonghe Wu, Liang Chen
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Abstract

Background: Tumorigenicity represents a critical challenge in stem cell-based therapies requiring rigorous monitoring. Conventional approaches for tumorigenicity evaluation are based on animal models and have numerous limitations. Brain organoids, which recapitulate the structural and functional complexity of the human brain, have been widely used in neuroscience research. However, the capacity of brain organoids for tumorigenicity evaluation needs to be further elucidated.

Methods: A cerebral organoid model produced from human pluripotent stem cells (hPSCs) was employed. Meanwhile, to enhance the detection sensitivity for potential tumorigenic cells, we created a glioblastoma-like organoid (GBM organoid) model from TP53-/-/PTEN-/- hPSCs to provide a tumor microenvironment for injected cells. Midbrain dopamine (mDA) cells from human embryonic stem cells were utilized as a cell therapy product. mDA cells, hPSCs, mDA cells spiked with hPSCs, and immature mDA cells were then injected into the brain organoids and NOD SCID mice. The injected cells within the brain organoids were characterized, and compared with those injected in vivo to evaluate the capability of the brain organoids for tumorigenicity evaluation. Single-cell RNA sequencing was performed to identify the differential gene expression between the cerebral organoids and the GBM organoids.

Results: Both cerebral organoids and GBM organoids supported maturation of the injected mDA cells. The hPSCs and immature mDA cells injected in the GBM organoids showed a significantly higher proliferative capacity than those injected in the cerebral organoids and in NOD SCID mice. Furthermore, the spiked hPSCs were detectable in both the cerebral organoids and the GBM organoids. Notably, the GBM organoids demonstrated a superior capacity to enhance proliferation and pluripotency of spiked hPSCs compared to the cerebral organoids and the mouse model. Kyoto Encyclopedia of Genes and Genomes analysis revealed upregulation of tumor-related metabolic pathways and cytokines in the GBM organoids, suggesting that these factors underlie the high detection sensitivity for tumorigenicity evaluation.

Conclusions: Our findings suggest that brain organoids could represent a novel and effective platform for evaluating the tumorigenic risk in stem cell-based therapies. Notably, the GBM organoids offer a superior platform that could complement or potentially replace traditional animal-based models for tumorigenicity evaluation.

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基于脑器官组织的细胞疗法致瘤性评估平台。
背景:肿瘤致病性是干细胞疗法面临的重大挑战,需要严格监测。传统的致瘤性评估方法以动物模型为基础,存在诸多局限性。脑器官模型再现了人脑结构和功能的复杂性,已广泛应用于神经科学研究。然而,脑器官组织用于肿瘤致病性评估的能力还有待进一步阐明:方法:采用人多能干细胞(hPSCs)制备的脑器官模型。同时,为了提高对潜在致瘤细胞的检测灵敏度,我们用TP53-/-/PTEN-/- hPSCs创建了胶质母细胞瘤样类器官(GBM organoid)模型,为注射细胞提供肿瘤微环境。然后将mDA细胞、hPSCs、添加了hPSCs的mDA细胞和未成熟的mDA细胞注射到脑器官组织和NOD SCID小鼠体内。对脑器官组织内注射的细胞进行鉴定,并与体内注射的细胞进行比较,以评估脑器官组织的致瘤性。对单细胞RNA进行测序,以确定脑组织器官和GBM组织器官之间的不同基因表达:结果:脑器质和GBM器质都支持注射的mDA细胞成熟。注射到GBM器官组织中的hPSCs和未成熟mDA细胞的增殖能力明显高于注射到大脑器官组织和NOD SCID小鼠体内的hPSCs和未成熟mDA细胞。此外,在脑组织器官和 GBM 组织器官中都能检测到添加的 hPSCs。值得注意的是,与脑器官组织和小鼠模型相比,GBM器官组织在增强加标hPSCs的增殖和多能性方面表现出更强的能力。京都基因和基因组百科全书》的分析显示,GBM组织器官中肿瘤相关代谢途径和细胞因子上调,这表明这些因素是肿瘤致性评估检测灵敏度高的原因:我们的研究结果表明,脑组织器官是评估干细胞疗法致瘤风险的新型有效平台。值得注意的是,GBM器官组织提供了一个优越的平台,可补充或有可能取代传统的动物模型进行致瘤性评估。
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来源期刊
Translational Neurodegeneration
Translational Neurodegeneration Neuroscience-Cognitive Neuroscience
CiteScore
19.50
自引率
0.80%
发文量
44
审稿时长
10 weeks
期刊介绍: Translational Neurodegeneration, an open-access, peer-reviewed journal, addresses all aspects of neurodegenerative diseases. It serves as a prominent platform for research, therapeutics, and education, fostering discussions and insights across basic, translational, and clinical research domains. Covering Parkinson's disease, Alzheimer's disease, and other neurodegenerative conditions, it welcomes contributions on epidemiology, pathogenesis, diagnosis, prevention, drug development, rehabilitation, and drug delivery. Scientists, clinicians, and physician-scientists are encouraged to share their work in this specialized journal tailored to their fields.
期刊最新文献
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