Role of Sodium-Dependent Vitamin C Transporter-2 and Ascorbate in Regulating the Hypoxic Pathway in Cultured Glioblastoma Cells.

IF 3 3区 生物学 Q3 BIOCHEMISTRY & MOLECULAR BIOLOGY Journal of cellular biochemistry Pub Date : 2024-10-09 DOI:10.1002/jcb.30658
Eleanor R Burgess, Citra Praditi, Elisabeth Phillips, Margreet C M Vissers, Bridget A Robinson, Gabi U Dachs, George A R Wiggins
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Abstract

The most common and aggressive brain cancer, glioblastoma, is characterized by hypoxia and poor survival. The pro-tumour transcription factor, hypoxia-inducible factor (HIF), is regulated via HIF-hydroxylases that require ascorbate as cofactor. Decreased HIF-hydroxylase activity triggers the hypoxic pathway driving cancer progression. Tissue ascorbate accumulates via the sodium-dependent vitamin C transporter-2 (SVCT2). We hypothesize that glioblastoma cells rely on SVCT2 for ascorbate accumulation, and that knockout of this transporter would disrupt the regulation of the hypoxic pathway by ascorbate. Ascorbate uptake was measured in glioblastoma cell lines (U87MG, U251MG, T98G) by high-performance liquid chromatography. CRISPR/Cas9 was used to knockout SVCT2. Cells were treated with cobalt chloride, desferrioxamine or 5% oxygen, with/without ascorbate, and key hypoxic pathway proteins were measured using Western blot analysis. Ascorbate uptake was cell line dependent, ranging from 1.7 to 11.0 nmol/106 cells. SVCT2-knockout cells accumulated 90%-95% less intracellular ascorbate than parental cells. The hypoxic pathway was induced by all three stimuli, and ascorbate reduced this induction. In the SVCT2-knockout cells, ascorbate had limited effect on the hypoxic pathway. This study verifies that intracellular ascorbate is required to suppress the hypoxic pathway. As patient survival is related to an activated hypoxic pathway, increasing intra-tumoral ascorbate may be of clinical interest.

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钠依赖性维生素 C 转运体-2 和抗坏血酸在调节培养胶质母细胞瘤细胞缺氧途径中的作用
胶质母细胞瘤是最常见的侵袭性脑癌,其特点是缺氧和生存率低。促肿瘤转录因子--缺氧诱导因子(HIF)通过 HIF-hydroxylases 调节,而 HIF-hydroxylases 需要抗坏血酸作为辅助因子。HIF-hydroxylase 活性的降低会引发缺氧途径,从而推动癌症的发展。组织中的抗坏血酸通过钠依赖性维生素 C 转运体-2(SVCT2)积累。我们假设胶质母细胞瘤细胞依赖 SVCT2 来积累抗坏血酸,而敲除该转运体将破坏抗坏血酸对缺氧途径的调节。通过高效液相色谱法测量了胶质母细胞瘤细胞系(U87MG、U251MG、T98G)对抗坏血酸的吸收。使用 CRISPR/Cas9 基因敲除 SVCT2。用氯化钴、去铁胺或 5%的氧气(含/不含抗坏血酸)处理细胞,并通过 Western 印迹分析测定缺氧通路的关键蛋白。抗坏血酸的吸收与细胞系有关,范围从1.7到11.0 nmol/106个细胞。与亲代细胞相比,SVCT2-基因敲除细胞积累的细胞内抗坏血酸减少了90%-95%。三种刺激都会诱导缺氧通路,而抗坏血酸会减少这种诱导。在 SVCT2 基因敲除的细胞中,抗坏血酸对缺氧通路的影响有限。这项研究验证了抑制缺氧通路需要细胞内的抗坏血酸。由于患者的存活与缺氧通路的激活有关,因此增加瘤内抗坏血酸可能具有临床意义。
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来源期刊
Journal of cellular biochemistry
Journal of cellular biochemistry 生物-生化与分子生物学
CiteScore
9.90
自引率
0.00%
发文量
164
审稿时长
1 months
期刊介绍: The Journal of Cellular Biochemistry publishes descriptions of original research in which complex cellular, pathogenic, clinical, or animal model systems are studied by biochemical, molecular, genetic, epigenetic or quantitative ultrastructural approaches. Submission of papers reporting genomic, proteomic, bioinformatics and systems biology approaches to identify and characterize parameters of biological control in a cellular context are encouraged. The areas covered include, but are not restricted to, conditions, agents, regulatory networks, or differentiation states that influence structure, cell cycle & growth control, structure-function relationships.
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