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Silibinin exerts sustained growth suppressive effect against human colon carcinoma SW480 xenograft by targeting multiple signaling molecules.

机译:通过靶向多个信号分子,硅藻土对人结肠癌SW480异种移植物施加持续的生长抑制作用。

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PURPOSE: Earlier, we reported the strong preventive efficacy of silibinin against colorectal cancer (CRC), but its usefulness against established CRC or effect of its withdrawal on CRC growth remained unknown. Present study focused on these important issues by employing two different treatment protocols in advanced human CRC SW480 xenograft in nude mice. METHODS: In the first treatment protocol, silibinin was fed for 28 days (200 mg/kg body weight, 5 days/week) to mice with growing SW480 xenograft; thereafter, tumor growth was monitored for additional 3 weeks without silibinin treatment. In the second protocol, silibinin treatment was started after 25 days of SW480 cells injection (established tumors), and tumor growth was studied 4 days, 8 days and 16 days after silibinin treatment. RESULTS: In both treatment protocols, silibinin had strong and sustained inhibitory effect on xenograft growth. Detailed xenograft analyses showed that silibinin, in both treatment protocols, exerts anti-proliferative, pro-apoptotic and anti-angiogenic effects. Further, silibinin reduced the expression of beta-catenin and phospho-GSK3beta in xenograft tissues. Silibinin also targeted signaling molecules involved in CRC proliferation and survival (cyclin D1, c-Myc and survivin) as well as angiogenesis regulators (VEGF and iNOS). CONCLUSIONS: Collectively, these findings substantiate silibinin's therapeutic efficacy against CRC, advocating its translational potential.
机译:目的:早些时候,我们报告了硅蛋白对结肠直肠癌(CRC)的强烈预防效果,但其对已建立的CRC或其戒断对CRC生长的影响仍然未知。目前研究专注于这些重要问题,通过在裸鼠中使用两种不同的治疗方案在裸鼠中使用两种不同的治疗方案。方法:在第一种处理方案中,硅蛋白将28天(200mg / kg体重,5天/周)加入小鼠,与生长SW480异种移植物;此后,在没有硅蛋白处理的情况下监测肿瘤生长另外3周。在第二方案中,在SW480细胞25天后开始硅蛋白处理(已建立的肿瘤),在硅蛋白处理后4天,8天和16天进行肿瘤生长。结果:在治疗方案中,硅蛋白对异种移植生长具有强烈且持续的抑制作用。详细的异种移植物分析表明,在治疗方案中,硅蛋白施加抗增殖性,促细胞凋亡和抗血管生成效果。此外,硅藻土在异种移植组织中降低了β-连环蛋白和磷酸磷酸酯和磷酸磷酸-GSK3β的表达。硅藻土还靶向CRC增殖和存活(细胞周期蛋白D1,C-MYC和Survivin)以及血管生成调节剂(VEGF和InOS)的信号传导分子。结论:集体,这些研究结果证实了硅蛋白对CRC的治疗效果,倡导其平移潜力。

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