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Cytotoxic and Anti-cancer Effects of Nickel Nanowires against Pancreatic Cancer Cells

机译:镍纳米线对胰腺癌细胞的细胞毒性和抗癌作用

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Cytotoxicity study of magnetic nanomaterials is a key consideration for biomedical applications. Very little is known about the cytotoxic and anti-cancer effects of nickel nanowires (Ni NWs) on mammalian cells and their interaction with proliferating cancer cells. Current therapeutics do not address the full heterogeneity of pancreatic cancers due to the resistance to apoptosis and does not suffice for a successful treatment. Therefore, synthesis of novel anticancer drugs continues to be a potential topic for pancreatic cancer research. In this study, we have investigated the cellular toxicity and anti-cancer effects of Ni NWs in one of the most aggressive human pancreatic ductal cancer (Panc-1) cell lines with the objective of development of a potential treatment strategy. Ni NWs were fabricated in a custom-made setup utilizing the electrodeposition method. Elemental analysis, crystallographic structure, and morphological properties of the synthesized Ni NWs were investigated using Energy Dispersive X-ray Analysis (EDAX), X-Ray Diffraction (X-RD) and Scanning Electron Microscopy (SEM), respectively. Panc-1 cell cultures were maintained according to a slightly modified American Type Culture Collection (ATCC) protocol. Morphological apoptogenic characteristics assessment of the Ni NWs induced Panc-1 cell was accomplished using phase contrast microscopy (PCM). Two commercially available cytotoxicity procedures including 3-(4, 5-dimethylthiazol-2-yl)-2, 5-diphenyl tetrazolium bromide (MTT) and trypan blue (TB) assays were utilized to determine the qualitative and quantitative cytotoxicity and anti-cancer effects of Ni NWs. As a negative control, Panc-1 cells without Ni NWs treatment were used in all experiments. Phase contrast microscopy (PCM) was used to confirm the Ni NWs internalization by Panc-1 cells. Both the MTT and TB assays, qualitatively and quantitatively confirmed the cytotoxic and anti-cancer effects of Ni NWs treated Panc-1 cells in vitro in both concentration and exposure-time dependent manners. We studied the cytotoxic and anti-cancer effects of Ni NWs on Panc-1 cells using novel integrated bionanotechnological approaches to understand the corresponding biological pathway with the objective of developing pancreatic cancer treatment. More specifically, we explored the molecular mechanisms associated with the pathway involved in Ni NWs induced toxicity against Panc-1 cells. Our results demonstrated that Ni NWs show strong candidacy for targeting cell selective applications in pancreatic cancer therapy.
机译:磁性纳米材料的毒性研究是生物医学应用的关键考虑因素。非常知之甚少对哺乳动物细胞镍纳米线(镍NWS)和它们与增殖癌细胞相互作用的细胞毒性和抗癌作用。目前的治疗没有解决胰腺癌的全异质性,由于凋亡的阻力和不足够了成功的治疗。因此,新型抗癌药物的合成仍然是胰腺癌研究潜在的课题。在这项研究中,我们已经与目标的一个潜在的治疗方法的发展的最积极的人胰腺导管癌(PANC-1)细胞系的一个研究镍纳米线的细胞毒性和抗癌作用。镍纳米线在利用电沉积法定制的设置进行制造。元素分析,晶体结构,并且将合成的镍纳米线的形态性质,使用能量色散X射线分析(EDAX)研究,X射线衍射(X-RD)和分别扫描电子显微镜(SEM),。 PANC-1细胞培养物根据略加修改美国典型培养物保藏中心(ATCC)协议保持。镍纳米线的形态促细胞凋亡特性评估诱导的Panc-1细胞,使用相差显微镜(PCM)来完成的。两种可商购的细胞毒性的程序,包括3-(4,5二甲基噻唑-2-基)-2,5-二苯基四唑溴化物(MTT)和台盼蓝(TB)测定法用于确定的定性和定量的细胞毒性和抗癌镍纳米线的影响。作为阴性对照,Panc-1细胞没有添加Ni的NW治疗在所有实验中使用。相差显微镜(PCM)被用于确认由Panc-1细胞的镍纳米线内化。无论是MTT和TB测定,定性和定量地证实镍纳米线的细胞毒性和抗癌作用在两种浓度和曝光时间依赖性处理Panc-1细胞在体外。我们使用新型集成bionanotechnological方法来了解与目标显影胰腺癌治疗的相应的生物学途径研究了Panc-1细胞的Ni纳米线的细胞毒性和抗癌作用。更具体地,我们研究了与涉及的Ni纳米线诱导的毒性对Panc-1细胞的途径相关的分子机制。我们的研究结果表明,镍纳米线显示了在胰腺癌治疗靶向细胞的选择性应用强大的候选人。

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