胶质瘤的发生是由 Oct3/4 调控网络协调的。

IF 1.3 4区 医学 Q4 CLINICAL NEUROLOGY
Journal of neurosurgical sciences Pub Date : 2024-04-01 Epub Date: 2021-08-03 DOI:10.23736/S0390-5616.21.05437-0
Tatyana N Ignatova, Hersh J Chaitin, Nickolay V Kukekov, Oleg N Suslov, Galina I Dulatova, Khalid A Hanafy, Frank D Vrionis
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引用次数: 0

摘要

多形性胶质母细胞瘤(GBM)是一种致命性脑肿瘤,具有发育分层表型异质性、耐药性和反复生长等特点。来自人类中枢神经系统(CNS)的神经干细胞(NSCs)和来自患者来源GBM(pdGSC)样本的胶质母细胞瘤干细胞在二维孔板和三维单克隆神经球培养系统(pdMNCS)中培养。pdMNCS模型有望建立相关的三维肿瘤环境,使悬浮神经球内的GBM细胞维持在干细胞阶段。利用pdMNCS,我们检测了GBM细胞系的各种发育癌干细胞标记,包括早期胚泡内细胞团(ICM)特异性Nanog、Oct3/4,B和CD133。我们观察到,胶质瘤球衍生细胞重现了 MNCS 表观遗传型。CD133是胶质细胞的标志物,在三维胶质球中表达旺盛,并定位于质膜区。相反,在传统二维培养条件下生长的胶质母球很快就失去了 CD133 的表达,这表明 CD133 的不同表达取决于细胞培养条件。重要的是,该实验证明患者衍生细胞的细胞骨架微管和中间丝(IFs)分化不完全,与市售的 GBM 细胞系类似。随后,为了确定Oct3/4是否为CD133表达和癌症干性所必需,我们用针对Oct3/4的siRNA转染了二维和三维培养物,发现胶质小球的形成明显减少。这些结果表明,Oct3/4,A和CD133的表达抑制了GSCs的分化。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
Gliomagenesis is orchestrated by the Oct3/4 regulatory network.

Background: Glioblastoma multiforme (GBM) is a lethal brain tumor characterized by developmental hierarchical phenotypic heterogeneity, therapy resistance and recurrent growth. Neural stem cells (NSCs) from human central nervous system (CNS), and glioblastoma stem cells from patient-derived GBM (pdGSC) samples were cultured in both 2D well-plate and 3D monoclonal neurosphere culture system (pdMNCS). The pdMNCS model shows promise to establish a relevant 3D-tumor environment that maintains GBM cells in the stem cell phase within suspended neurospheres.

Methods: Utilizing the pdMNCS, we examined GBM cell-lines for a wide spectrum of developmental cancer stem cell markers, including the early blastocyst inner-cell mass (ICM)-specific Nanog, Oct3/4,B, and CD133.

Results: We observed that MNCS epigenotype is recapitulated using gliomasphere-derived cells. CD133, the marker of GSC is robustly expressed in 3D-gliomaspheres and localized within the plasma membrane compartment. Conversely, gliomasphere cultures grown in conventional 2D culture quickly lost CD133 expression, indicating its variable expression is dependent on cell-culture conditions. Incomplete differentiation of cytoskeleton microtubules and intermediate filaments (IFs) of patient derived cells, similar to commercially available GBM cell lines, was seen. Subsequently, in order to determine whether Oct3/4 it was necessary for CD133 expression and cancer stemness, we transfected 2D and 3D culture with siRNA against Oct3/4 and found a significant reduction in gliomasphere formation.

Conclusions: These results suggest that expression of Oct3/4,A- and CD133 suppress differentiation of GSCs.

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来源期刊
Journal of neurosurgical sciences
Journal of neurosurgical sciences CLINICAL NEUROLOGY-SURGERY
CiteScore
3.00
自引率
5.30%
发文量
202
审稿时长
>12 weeks
期刊介绍: The Journal of Neurosurgical Sciences publishes scientific papers on neurosurgery and related subjects (electroencephalography, neurophysiology, neurochemistry, neuropathology, stereotaxy, neuroanatomy, neuroradiology, etc.). Manuscripts may be submitted in the form of ditorials, original articles, review articles, special articles, letters to the Editor and guidelines. The journal aims to provide its readers with papers of the highest quality and impact through a process of careful peer review and editorial work.
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