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Gold-chrysophanol nanoparticles suppress human prostate cancer progression through inactivating AKT expression and inducing apoptosis and ROS generation in vitro and in vivo

机译：金-酚金纳米颗粒通过失活AKT表达并诱导体内和体外凋亡和ROS产生来抑制人类前列腺癌的进展

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Controlled releasing of regulations remains the most convenient method to deliver various drugs. In the present study, we precipitated gold nanoparticles with chrysophanol. The gold-chrysophanol into poly (DL-lactide-co-glycolide) nanoparticles was loaded and the biological activity of chrysophanol nanoparticles on human LNCap prostate cancer cells, was tested to acquire the sustained releasing property. The circular dichroism spectroscopy indicated that chrysophanol nanoparticles effectively resulted in conformational alterations in DNA and regulated different proteins associated with cell cycle arrest. The reactive oxygen species (ROS), apoptosis, cell cycle, DNA damage, Cyto-c and caspase-3 activity were analyzed, and the expression levels of different anti- and pro-apoptotic were studied using immunoblotting analysis. The cytotoxicity assay suggested that chrysophanol nanoparticles preferentially killed prostate cancer cells in comparison to the normal cells. Chrysophanol nanoparticles reduced histone deacetylases (HDACs) to suppress cell proliferation and induce apoptosis by arresting the cell cycle in sub-G phase. In addition, the cell cycle-related proteins, including p27, CHK1, cyclin D1, CDK1, p-AMP-activated protein kinase (AMPK) and p-protein kinase B (AKT), were regulated by chrysophanol nanoparticles to prevent human prostate cancer cell progression. Chrysophanol nanoparticles induced apoptosis in LNCap cells by promoting p53/ROS crosstalk to prevent proliferation. Pharmacokinetic study in mice indicated that chrysophanol nanoparticle injection showed high bioavailability compared to the free chrysophanol. Also, in vivo study revealed that chrysophanol nanoparticles obviously reduced tumor volume and weight. In conclusion, the data above suggested that chrysophanol nanoparticles might be effective to prevent human prostate cancer progression.

机译：法规的受控发布仍然是交付各种药物的最便捷方法。在本研究中，我们用车酚醇沉淀了金纳米颗粒。负载金-酚金到聚（DL-丙交酯-共-乙交酯）纳米粒子中，并测试了酚金纳米粒子对人LNCap前列腺癌细胞的生物学活性，以获得持续释放性能。圆二色光谱表明，chsophophanol纳米粒子有效地导致DNA的构象改变，并调节与细胞周期阻滞有关的不同蛋白质。分析了活性氧（ROS），细胞凋亡，细胞周期，DNA损伤，Cyto-c和caspase-3活性，并通过免疫印迹分析了不同抗凋亡和促凋亡的表达水平。细胞毒性测定表明，与正常细胞相比，车酚醇纳米颗粒优先杀死前列腺癌细胞。酚酞纳米颗粒通过将细胞周期停滞在亚G期来减少组蛋白脱乙酰基酶（HDACs），从而抑制细胞增殖并诱导细胞凋亡。此外，甲壳ry酚纳米粒调节与细胞周期相关的蛋白，包括p27，CHK1，cyclin D1，CDK1，p-AMP激活的蛋白激酶（AMPK）和p-蛋白激酶B（AKT），以预防人类前列腺癌。细胞进程。 ry酚纳米粒通过促进p53 / ROS串扰阻止增殖而诱导LNCap细胞凋亡。小鼠体内的药代动力学研究表明，与游离的chsophophanol相比，chsophophanol纳米颗粒注射剂具有较高的生物利用度。此外，体内研究表明，金鳞酚纳米颗粒明显降低了肿瘤的体积和重量。总之，以上数据表明，chsophophanol纳米粒子可能有效预防人类前列腺癌的进展。

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期刊名称 International Journal of Oncology
作者
Li Lu; Ke Li; Yun-Hua Mao; Hu Qu; Bing Yao; Wen-Wen Zhong; Bo Ma; Zhong-Yang Wang;
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作者单位

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年(卷),期 -1(51),4
年度 -1
页码 1089–1103
总页数 15
原文格式 PDF
正文语种
中图分类肿瘤学;
关键词
chrysophanol nanoparticles prostate cancer apoptosis ROS bioavailability;

机译：ry酚纳米粒;前列腺癌;细胞凋亡;活性氧;生物利用度;

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专利

1. Plant flavonoid apigenin inactivates Akt to trigger apoptosis in human prostate cancer: an in vitro and in vivo study. [J] . Kaur P, Shukla S, Gupta S Carcinogenesis . 2008,第11期

机译：体外和体内研究表明，植物类黄酮芹菜素可以使Akt失活，从而触发人类前列腺癌的凋亡。
2. Plant flavonoid apigenin inactivates Akt to trigger apoptosis in human prostate cancer: an in vitro and in vivo study [J] . Parminder Kaur1 Sanjeev Shukla1 and Sanjay Gupta123 Carcinogenesis . 2008,第11期

机译：植物类黄酮芹菜素能灭活Akt触发人类前列腺癌的细胞凋亡：一项体内外研究
3. HIV-1 protease inhibitor induces growth arrest and apoptosis of human prostate cancer LNCaP cells in vitro and in vivo in conjunction with blockade of androgen receptor STAT3 and AKT signaling. [J] . Yang Y, Ikezoe T, Takeuchi T, Cancer science. . 2005,第7期

机译：HIV-1蛋白酶抑制剂与雄激素受体STAT3和AKT信号传导阻滞一起，在体外和体内诱导人前列腺癌LNCaP细胞的生长停滞和凋亡。
4. Development of In Vitro Prostate Cancer Biomarkers on the Basis of Gelatin Matrix Incorporated Gold Nanoparticles Functionalized with Fluorescence Dye and Prostate Specific Membrane Antigen [C] . K. CHUBINIDZE, B. PARTSVANIA, A. KHUSKIVADZE, International Caucasian Symposium on Polymers and Advanced Materials . 2020

机译：基于明胶基质的体外前列腺癌生物标志物的发展掺入了用荧光染料和前列腺特异性膜抗原官能化的金纳米颗粒
5. Potato and grape polyphenols, respectively, suppress high-fat diet-elevated oxidative stress/innate inflammation markers in porcine model and induce apoptosis in HCT-116 p53 +/+ and p53 -/- human colon cancer cell lines in vitro. [D] . Radhakrishnan, Sridhar. 2014

机译：马铃薯和葡萄中的多酚分别抑制猪模型中高脂饮食升高的氧化应激/先天性炎症标记，并在体外诱导HCT-116 p53 + / +和p53-/-人结肠癌细胞系中的凋亡。
6. Plant flavonoid apigenin inactivates Akt to trigger apoptosis in human prostate cancer: an in vitro and in vivo study [O] . Parminder Kaur, Sanjeev Shukla, Sanjay Gupta -1

机译：植物类黄酮芹菜素能灭活Akt触发人类前列腺癌的细胞凋亡：一项体内外研究
7. Plant flavonoid apigenin inactivates Akt to trigger apoptosis in human prostate cancer: an in vitro and in vivo study [O] . Kaur, Parminder, Shukla, Sanjeev, Gupta, Sanjay 2008

机译：植物类黄酮芹菜素能灭活Akt触发人类前列腺癌的细胞凋亡：一项体内外研究
8. Molecular Determinants of Prostate Cancer Progression Across Race- Ethnicity. Project A - The Human 5RD5A2 Gene and Prostate Cancer Progression. Project B - Androgen Receptor (AR) Signaling in Prostate Cancer Progression. Project C - Cellular and Molecular Markers of Prostate Cancer Progression Core - Epidemiology Core [R] . Ross, R. R. , Reichardt, J. , Coetzee, G. A. , 2002

机译：跨越种族的前列腺癌进展的分子决定因素。项目a - 人类5RD5a2基因和前列腺癌进展。项目B - 雄激素受体（aR）在前列腺癌进展中的信号传导。项目C - 前列腺癌进展核心的细胞和分子标记 - 流行病学核心

Gold-chrysophanol nanoparticles suppress human prostate cancer progression through inactivating AKT expression and inducing apoptosis and ROS generation in vitro and in vivo

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