抗坏血酸盐的可利用性会影响肿瘤植入成功率,并增加古洛糖酸内酯氧化酶基因敲除小鼠的肿瘤排斥反应。
Ascorbate availability affects tumor implantation-take rate and increases tumor rejection in Gulo mice.
作者信息
Campbell Elizabeth J, Vissers Margreet Cm, Dachs Gabi U
机构信息
Mackenzie Cancer Research Group.
Centre for Free Radical Research, Department of Pathology, University of Otago, Christchurch, New Zealand.
出版信息
Hypoxia (Auckl). 2016 Apr 8;4:41-52. doi: 10.2147/HP.S103088. eCollection 2016.
In solid tumors, HIF1 upregulates the expression of hundreds of genes involved in cell survival, tumor growth, and adaptation to the hypoxic microenvironment. HIF1 stabilization and activity are suppressed by prolyl and asparagine hydroxylases, which require oxygen as a substrate and ascorbate as a cofactor. This has led us to hypothesize that intracellular ascorbate availability could modify the hypoxic HIF1 response and influence tumor growth. In this study, we investigated the effect of variable intracellular ascorbate levels on HIF1 induction in cancer cells in vitro, and on tumor-take rate and growth in the Gulo mouse. These mice depend on dietary ascorbate, and were supplemented with 3,300 mg/L, 330 mg/L, or 33 mg/L ascorbate in their drinking water, resulting in saturating, medium, or low plasma and tissue ascorbate levels, respectively. In Lewis lung carcinoma cells (LL/2) in culture, optimal ascorbate supplementation reduced HIF1 accumulation under physiological but not pathological hypoxia. LL/2, B16-F10 melanoma, or CMT-93 colorectal cancer cells were implanted subcutaneously into Gulo mice at a range of cell inocula. Establishment of B16-F10 tumors in mice supplemented with 3,300 mg/L ascorbate required an increased number of cancer cells to initiate tumor growth compared with the number of cells required in mice on suboptimal ascorbate intake. Elevated ascorbate intake was also associated with decreased tumor ascorbate levels and a reduction in HIF1α expression and transcriptional activity. Following initial growth, all CMT-93 tumors regressed spontaneously, but mice supplemented with 33 mg/L ascorbate had lower plasma ascorbate levels and grew larger tumors than optimally supplemented mice. The data from this study indicate that improved ascorbate intake is consistent with increased intracellular ascorbate levels, reduced HIF1 activity and reduced tumor initiation and growth, and this may be advantageous in the management of cancer.
在实体瘤中,低氧诱导因子1(HIF1)上调数百种参与细胞存活、肿瘤生长以及适应缺氧微环境的基因的表达。脯氨酰和天冬酰胺羟化酶可抑制HIF1的稳定性和活性,这两种酶均需要氧气作为底物,维生素C作为辅助因子。这使我们推测细胞内维生素C的可利用性可能会改变缺氧状态下的HIF1反应并影响肿瘤生长。在本研究中,我们调查了细胞内维生素C水平变化对体外癌细胞中HIF1诱导作用的影响,以及对古洛糖酸内酯氧化酶(Gulo)基因敲除小鼠的肿瘤接种率和生长的影响。这些小鼠依赖饮食中的维生素C,在其饮用水中分别补充3300 mg/L、330 mg/L或33 mg/L的维生素C,结果分别导致血浆和组织中维生素C水平达到饱和、中等或较低。在培养的Lewis肺癌细胞(LL/2)中,最佳的维生素C补充可在生理性而非病理性缺氧条件下减少HIF1的积累。将LL/2、B16-F10黑色素瘤或CMT-93结肠癌细胞以一系列细胞接种量皮下植入Gulo小鼠体内。与维生素C摄入不足的小鼠相比,补充3300 mg/L维生素C的小鼠中,B16-F10肿瘤的形成需要更多数量的癌细胞才能启动肿瘤生长。维生素C摄入量的增加还与肿瘤中维生素C水平的降低以及HIF1α表达和转录活性的降低有关。在初始生长之后,所有CMT-93肿瘤均自发消退,但补充33 mg/L维生素C的小鼠血浆维生素C水平较低,且肿瘤生长比最佳补充维生素C的小鼠更大。本研究数据表明,维生素C摄入量的增加与细胞内维生素C水平的升高、HIF1活性的降低以及肿瘤起始和生长的减少相一致,这在癌症管理中可能具有优势。
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