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首页> 外文期刊>Journal of Cancer Therapy >Enhancement of Tumor Regression by Coulomb Nanoradiator Effect in Proton Treatment of Iron-Oxide Nanoparticle-Loaded Orthotopic Rat Glioma Model: Implication of Novel Particle Induced Radiation Therapy
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Enhancement of Tumor Regression by Coulomb Nanoradiator Effect in Proton Treatment of Iron-Oxide Nanoparticle-Loaded Orthotopic Rat Glioma Model: Implication of Novel Particle Induced Radiation Therapy

机译:用库仑纳米辐射效应增强质子治疗氧化铁纳米粒子负载原位大鼠脑胶质瘤模型的肿瘤消退:新型粒子诱导放射治疗的意义

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Background: Proton-impact metallic nanoparticles, inducing low-energy electrons emission and characteristic X-rays termed as Coulomb nanoradiator effect (CNR), are known to produce therapeutic enhancement in proton treatment on experimental tumors. The purpose of this pilot study was to investigate the effect of CNR-based dose enhancement on tumor growth inhibition in an iron-oxide nanoparticle (FeONP)-loaded orthotopic rat glioma model. Methods: Proton-induced CNR was exploited to treat glioma-bearing SD rat loaded with FeONP by either fully-absorbed single pristine Bragg peak (APBP) or spread-out Bragg peak (SOBP) 45-MeV proton beam. A selected number of rats were examined by MRI before and after treatment to obtain the size and position information for adjusting irradiation field. Tumor regression assay was performed by histological analysis of residual tumor in the sacrificed rats 7 days after treatment. The results of CNR-treated groups were compared with the proton alone control. Results: Intravenous injection of FeONP (300 mg/kg) elevated the tumor concentration of iron up to 37 μg of Fe/g tissue, with a tumor-to-normal ratio of 5, 24 hours after injection. The group receiving FeONP and proton beam showed 65% - 79% smaller tumor volume dose-dependently compared with the proton alone group. The rats receiving FeONP and controlled irradiation field by MR imaging demonstrated more than 95% - 99% tumor regression compared with MRI-determined initial tumor size. Conclusions: Proton-impact FeONP produced therapeutic enhancement compared with proton alone in an orthotopic rat glioma model at a selected temporal point after treatment. Single BP proton beam could induce CNR- based dose enhancement and produce enhanced tumor regression that was comparable to SOBP treatment despite inhomogeneous tumor dose in the APBP-treated tumor. These results may suggest emergence of novel Particle Induced Radiation Therapy (PIRT) on malignant glioma.
机译:背景:质子撞击的金属纳米粒子会诱导低能电子发射,并具有称为库仑纳米辐射效应(CNR)的特征性X射线,可在质子治疗实验性肿瘤中产生治疗效果。这项初步研究的目的是研究基于CNR的剂量增加在负载铁氧化物纳米颗粒(FeONP)的原位大鼠神经胶质瘤模型中对肿瘤生长抑制的影响。方法:利用质子诱导的CNR通过完全吸收的单个原始Bragg峰(APBP)或散布的Bragg峰(SOBP)45-MeV质子束治疗载有FeONP的神经胶质瘤SD大鼠。在治疗之前和之后通过MRI检查选定数目的大鼠,以获得用于调节照射场的大小和位置信息。治疗7天后,通过处死大鼠的残余肿瘤的组织学分析进行肿瘤消退测定。将CNR治疗组的结果与单独质子对照组进行比较。结果:静脉注射FeONP(300 mg / kg)可将铁的肿瘤浓度提高至37μgFe / g组织,注射后24小时的肿瘤与正常比例为5。与单独的质子组相比,接受FeONP和质子束治疗的组显示出剂量依赖性地减小了65%-79%的肿瘤体积。与MRI确定的初始肿瘤大小相比,接受FeONP并通过MR成像控制照射场的大鼠显示出超过95%-99%的肿瘤消退。结论:在治疗后的选定时间点,在原位大鼠神经胶质瘤模型中,质子撞击FeONP与单独质子相比产生了治疗增强作用。单个BP质子束可以诱导基于CNR的剂量增强,并产生增强的肿瘤消退,这与SOBP治疗相当,尽管在APBP治疗的肿瘤中肿瘤剂量不均匀。这些结果可能表明出现了针对恶性神经胶质瘤的新型粒子诱导放射治疗(PIRT)。

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