首页> 外文期刊>Cancer Biochemistry Biophysics: Devoted to the Rapid Communication of Findings in Biochemistry and Biophysics Pertinent to the Knowledge of Cancer >Effect of vitamin C on androgen independent prostate cancer cells (PC3 and Mat-Ly-Lu) in vitro: involvement of reactive oxygen species-effect on cell number, viability and DNA synthesis.
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Effect of vitamin C on androgen independent prostate cancer cells (PC3 and Mat-Ly-Lu) in vitro: involvement of reactive oxygen species-effect on cell number, viability and DNA synthesis.

机译:维生素C对雄激素的影响独立前列腺癌细胞(生物和Mat-Ly-Lu)体外:活性氧的参与species-effect细胞数量、可行性和DNA合成。

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摘要

Studies have described the protective role of vitamin C (ascorbic acid) in certain types of cancer. In this study, we report the effects of vitamin C treatment of two androgen independent prostate cancer cell lines from human (PC3) and rat (Mat-Ly-Lu or MLL) sources. In vitro treatment of PC3 and MLL with sodium ascorbate acid (0-10 mM) resulted in a decrease in cell viability and thymidine incorporation into DNA. These effects of vit. C were dose and time dependent. Ascorbate induced these changes through the production of hydrogen peroxide since addition of catalase (100-300 units/ml), an enzyme that degrades hydrogen peroxide, inhibited the effects of ascorbate on these cell lines. In contrast, superoxide dismutase, an enzyme that dismutates superoxide and generates hydrogen peroxide did not prevent ascorbate-induced changes emphasizing the involvement of reactive oxygen species (ROS) in cellular damage. That singlet oxygen scavengers such as sodium azide and hydroquinone, hydroxyl radical scavengers such as D-mannitol and DL-alpha-tocopherol did not counteract the effects of ascorbate on thymidine incorporation suggests that these free radicals are not involved in cellular damage. In conclusion, these results suggest that vitamin C inhibits tumor growth by virtue of producing reactive oxygen species. These results suggest that ascorbate is a potent anticancer agent for prostate cancer cells.
机译:研究描述的防护作用维生素C(抗坏血酸)在某些类型的癌症。维生素C治疗两个雄激素独立前列腺癌从人类(生物)和细胞系老鼠(Mat-Ly-Lu或MLL)来源。与抗坏血酸钠治疗,生物和MLL酸(清廉毫米)导致细胞减少可行性和胸苷并入DNA。这些维生素的影响。相关的。通过过氧化氢的生产添加过氧化氢酶(100 - 300单位/毫升)过氧化氢酶,降解,抑制抗坏血酸盐在这些细胞株的影响。之下,一种酶,这种酶超氧化物歧化酶dismutates超氧化物并生成氢气过氧化并没有阻止ascorbate-induced改变强调被动的参与氧物种(ROS)的细胞损伤。单线态氧拾荒者如叠氮化钠和对苯二酚,氢氧自由基拾荒者D-mannitol和DL-alpha-tocopherol等不消除抗坏血酸盐的影响胸腺嘧啶核苷掺入表明这些免费自由基不参与细胞损伤。结论,这些结果表明,维生素C抑制肿瘤生长的生产活性氧物种。抗坏血酸盐是一种有效的抗癌剂前列腺癌的细胞。

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