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Gold Nanoshell mediated Hyperthermia enhances the efficacy of Radiation Therapy

机译:金纳米壳介导的热疗可增强放射治疗的功效

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Despite convincing evidence for hyperthermic radiosensitization, the invasive means of achieving and monitoring hyperthermia and the lack of good thermal dosimetry have hindered its use in routine clinical practice. A non-invasive method to generate and monitor hyperthermia would provide renewed enthusiasm for such treatments. Near-infrared absorbing gold nanoshells have been shown to accumulate preferentially in tumors via the enhanced permeability and retention effect and have been used for thermal ablation of tumors. We evaluated the use of these nanoshells to generate hyperthermia to evaluate the anti-tumor effects of combining gold nanoshell mediated hyperthermia with radiotherapy. Laser settings were optimized for hyperthermia in a mouse xenograft model to achieve a temperature rise of 40- 41℃ in the tumor periphery and 37-38℃ (AT=4-5℃) deeper within the tumors. The AT measurements were verified using both thermocouple and magnetic resonance thermal imaging (MRTI) temperature measurements. Tumor re-growth delay was estimated by measuring tumor size after treatment with radiation (10Gy single dose), hyperthermia (15 minutes at 40℃), and hyperthermia followed by radiation and control. Significant difference (p < 0.05) in the tumor volume doubling time was observed between the radiation group (13 days) and combination treatment group (25 days). The immunofluorescence staining for the hypoxic, proliferating cells and the vasculature corroborated our hypothesis that the radiosensitization is in part mediated by increased initial perfusion and subsequent collapse of vasculature that leads to acute inflammatory response in the tumor. The increased vascular perfusion immediately after gold nanoshell mediated hyperthermia is confirmed by dynamic contrast enhanced magnetic resonance imaging.
机译:尽管有令人信服的高温放射增敏证据,但实现和监测高温的侵入性手段以及缺乏良好的热剂量测定法阻碍了其在常规临床实践中的使用。产生和监测热疗的非侵入性方法将为这种治疗提供新的热情。已显示,近红外吸收金纳米壳通过增强的渗透性和保留效应优先在肿瘤中蓄积,并已用于肿瘤的热消融。我们评估了使用这些纳米壳产生高温来评估金纳米壳介导的高温与放疗相结合的抗肿瘤作用。针对小鼠异种移植模型中的热疗优化了激光设置,以使肿瘤周围温度升高40-41℃,使肿瘤内部温度升高37-38℃(AT = 4-5℃)。使用热电偶和磁共振热成像(MRTI)温度测量值验证了AT测量值。放射线治疗(单剂量10Gy),体温过高(40℃15分钟),体温过高以及放射线和对照治疗后,通过测量肿瘤大小来估计肿瘤的重生延迟。在放疗组(13天)和联合治疗组(25天)之间观察到肿瘤体积加倍时间有显着差异(p <0.05)。缺氧,增生细胞和脉管系统的免疫荧光染色证实了我们的假设,即放射增敏部分是由增加的初始灌注和随后的脉管系统塌陷介导的,从而导致肿瘤中的急性炎症反应。动态对比增强磁共振成像证实了金纳米壳介导的热疗后立即增加的血管灌注。

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