氧调节RS0 sdh缺陷嗜铬细胞瘤细胞系的增殖和表型。

Endocrine-related cancer Pub Date : 2025-06-03 Print Date: 2025-06-01 DOI:10.1530/ERC-25-0022
James F Powers, Brent Cochran, James D Baleja, Inna Lomakin, Xue Zhang, Annette Shepard-Barry, Arthur S Tischler
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引用次数: 0

摘要

RS0细胞系是大鼠来源的嗜铬细胞瘤细胞系,是研究由SDHB基因遗传突变引起的嗜铬细胞瘤/副神经节瘤的模型。先前的研究表明,RS0亲本肿瘤的异种移植物复制了其人类同类肿瘤的特征,包括SDHB的缺失和EPAS1/HIF2A激活的缺氧信号通路中基因的上调。细胞系的建立需要较低的O2浓度,因为在传统的20% O2的细胞培养气氛中细胞增殖被阻止。本研究描述了20%与5% O2和EPAS1/HIF2A抑制剂对RS0细胞表型的影响,并测试了在这些影响下培养的RS0细胞与它们的母体异种移植物和正常大鼠肾上腺髓质的比较。细胞培养中的O2浓度几乎影响细胞生物学的各个方面,最明显的是增殖,但也影响超微结构、转录组、代谢和内分泌功能。当维持在低氧环境时,细胞与异种移植物最相似,但体内和体外细胞之间的一些差异尚未完全解释。在高氧条件下下调的基因主要与细胞周期相关,而在低氧条件下上调的基因包括干细胞和神经元祖细胞标记物,这些标记物可能有助于细胞系的建立,以及人类嗜铬细胞瘤/副神经节瘤中表达的药物靶点。目前考虑用于治疗转移性sdh缺陷PPGL的EPAS1/HIF2A抑制剂可以模拟高氧的一些作用,而其他抑制剂可能与hif无关。EPAS1/HIF2A抑制剂的细胞抑制作用是可逆的,这表明它们作为单一疗法的有效性可能存在局限性。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
Oxygen regulates proliferation and phenotype in the RS0 SDH-deficient pheochromocytoma cell line.

The RS0 cell line is a rat-derived pheochromocytoma line developed as a model to study pheochromocytoma/paraganglioma caused by hereditary mutations of the SDHB gene. Previous studies demonstrated that xenografts of the RS0 parent tumor replicate characteristics of their human counterparts, including loss of SDHB and upregulation of genes in hypoxia signaling pathways activated by EPAS1/HIF2A. Establishment of the cell line required a low O2 concentration, as cell proliferation was arrested in a traditional cell culture atmosphere of 20% O2. The present study profiled the effects of 20% versus 5% O2 and EPAS1/HIF2A inhibitors on the RS0 cell phenotype and tested how RS0 cells cultured under these influences compare to their parent xenografts and normal rat adrenal medulla. O2 concentration in cell cultures influences almost every aspect of the cells' biology, most obviously proliferation but also ultrastructure, transcriptome, metabolism and endocrine function. The cells most closely resemble their xenografts when maintained in a low O2 environment, but some differences between the cells in vivo and in vitro are not fully explained. Genes downregulated in high O2 are predominantly associated with the cell cycle, while those upregulated in low O2 include stemness and neuronal progenitor markers that may have contributed to the establishment of the cell line, as well as drug targets expressed in human pheochromocytoma/paraganglioma. Some effects of high O2 are mimicked by EPAS1/HIF2A inhibitors currently considered for treatment of metastatic Sdh-deficient PPGL, while others may be HIF-independent. The cytostatic effect of EPAS1/HIF2A inhibitors is reversible, suggesting possible limits to their usefulness as monotherapies.

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