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Differential antitumor effects of vitamin D analogues on colorectal carcinoma in culture

机译:维生素D类似物对培养中大肠癌的差异抗肿瘤作用

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摘要

Colorectal cancer (CRC) is an emerging global problem with the rapid increase in its incidence being associated with an unhealthy lifestyle. Epidemiological studies have shown that decreased levels of vitamin D3 significantly increases the risk of CRC. Furthermore, negative effects of vitamin D3 deficiency can be compensated by appropriate supplementation. Vitamin D3 was shown to inhibit growth and induce differentiation of cancer cells, however, excessive vitamin D3 intake leads to hypercalcemia. Thus, development of efficient vitamin D3 analogues with limited impact on calcium homeostasis is an important scientific and clinically relevant task. The aims of the present study were to compare the antiproliferative potential of classic vitamin D3 metabolites (1α,25(OH)2D3 and 25(OH)D3) with selected low calcemic analogues (calcipotriol and 20(OH)D3) on CRC cell lines and to investigate the expression of vitamin D-related genes in CRC cell lines and clinical samples. Vitamin D3 analogues exerted anti-proliferative effects on all CRC cell lines tested. Calcipotriol proved to be as potent as 1α,25(OH)2D3 and had more efficacy than 20-hydroxyvitamin D3. In addition, the analogs tested effectively inhibited the formation of colonies in Matrigel. The expression of genes involved in 1α,25(OH)2D3 signaling and metabolism varied in cell lines analysed, which explains in part their different sensitivities to the various analogues. In CRC biopsies, there was decreased VDR expression in tumor samples in comparison to the surgical margin and healthy colon samples (P<0.01). The present study indicates that vitamin D3 analogues which have low calcemic activity, such as calcipotriol or 20(OH)D3, are very promising candidates for CRC therapy. Moreover, expression profiling of vitamin D-related genes is likely to be a powerful tool in the planning of anticancer therapy. Decreased levels of VDR and increased CYP24A1 expression in clinical samples underline the importance of deregulation of vitamin D pathways in the development of CRC.
机译:大肠癌(CRC)是一个正在出现的全球性问题,其发病率的快速上升与不健康的生活方式有关。流行病学研究表明,维生素D3含量降低会大大增加患CRC的风险。此外,维生素D3缺乏症的负面影响可以通过适当的补充来弥补。维生素D3被证明可抑制癌细胞生长并诱导癌细胞分化,但是,维生素D3摄入过多会导致高钙血症。因此,开发对钙动态平衡影响有限的有效维生素D3类似物是一项重要的科学和临床相关任务。本研究的目的是比较经典维生素D3代谢产物(1α,25(OH)2D3和25(OH)D3)与选定的低钙血症类似物(钙三醇和20(OH)D3)在CRC细胞系中的抗增殖潜力并研究维生素D相关基因在CRC细胞系和临床样品中的表达。维生素D3类似物对所有测试的CRC细胞系均具有抗增殖作用。卡泊三醇被证明与1α,25(OH)2D3一样有效,并且比20-羟基维生素D3具有更高的功效。此外,测试的类似物有效抑制了基质胶中菌落的形成。在所分析的细胞系中,参与1α,25(OH)2D3信号传导和代谢的基因的表达各不相同,这部分解释了它们对各种类似物的不同敏感性。在CRC活检中,与手术切缘和健康结肠样本相比,肿瘤样本中的VDR表达降低(P <0.01)。本研究表明,具有低钙血症活性的维生素D 3 类似物,如卡泊三醇或20(OH)D 3 ,是CRC治疗的非常有希望的候选者。此外,维生素D相关基因的表达谱分析可能是抗癌治疗规划中的有力工具。临床样品中VDR水平的降低和CYP24A1表达的增加强调了维生素D通路的失调在CRC发生中的重要性。

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