Establishment of tumor microenvironment-preserving organoid model from patients with intracranial meningioma

类有机物 脑膜瘤 肿瘤微环境 癌症研究 医学 免疫组织化学 细胞培养 脑瘤 病理 生物 细胞生物学 肿瘤细胞 遗传学
作者
Dokyeong Kim,Junseong Park,Hyeon‐Chun Park,Songzi Zhang,Minyoung Park,Soon A Park,Sug Hyung Lee,Youn Soo Lee,Jae‐Sung Park,Sin‐Soo Jeun,Yeun‐Jun Chung,Stephen Ahn
出处
期刊:Cancer Cell International [BioMed Central]
卷期号:24 (1) 被引量:8
标识
DOI:10.1186/s12935-024-03225-4
摘要

Abstract Background Although meningioma is the most common primary brain tumor, treatments rely on surgery and radiotherapy, and recurrent meningiomas have no standard therapeutic options due to a lack of clinically relevant research models. Current meningioma cell lines or organoids cannot reflect biological features of patient tumors since they undergo transformation along culture and consist of only tumor cells without microenvironment. We aim to establish patient-derived meningioma organoids (MNOs) preserving diverse cell types representative of the tumor microenvironment. Methods The biological features of MNOs were evaluated using WST, LDH, and collagen-based 3D invasion assays. Cellular identities in MNOs were confirmed by immunohistochemistry (IHC). Genetic alteration profiles of MNOs and their corresponding parental tumors were obtained by whole-exome sequencing. Results MNOs were established from four patients with meningioma (two grade 1 and two grade 2) at a 100% succession rate. Exclusion of enzymatic dissociation-reaggregation steps endowed MNOs with original histology and tumor microenvironment. In addition, we used a liquid media culture system instead of embedding samples into Matrigel, resulting in an easy-to-handle, cost-efficient, and time-saving system. MNOs maintained their functionality and morphology after long-term culture (> 9 wk) and repeated cryopreserving-recovery cycles. The similarities between MNOs and their corresponding parental tumors were confirmed by both IHC and whole-exome sequencing. As a representative application, we utilized MNOs in drug screening, and mifepristone, an antagonist of progesterone receptor, showed prominent antitumor efficacy with respect to viability, invasiveness, and protein expression. Conclusion Taken together, our MNO model overcame limitations of previous meningioma models and showed superior resemblance to parental tumors. Thus, our model could facilitate translational research identifying and selecting drugs for meningioma in the era of precision medicine.
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