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Hybrid Manganese Dioxide Nanoparticles Potentiate Radiation Therapy by Modulating Tumor Hypoxia

机译:混合二氧化锰纳米粒子通过调节肿瘤缺氧增强放射治疗。

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Hypoxia in the tumor microenvironment (TME) mediates resistance to radiotherapy and contributes to poor prognosis in patients receiving radiotherapy. Here we report the design of clinically suitable formulations of hybrid manganese dioxide (MnO2) nanoparticles (MDNP) using biocompatible materials to reoxygenate the TME by reacting with endogenous H2O2. MDNP containing hydrophilic terpolymer-protein-MnO2 or hydrophobic polymer-lipid-MnO2 provided different oxygen generation rates in the TME relevant to different clinical settings. In highly hypoxic murine or human xenograft breast tumor models, we found that administering either MDNP formulation before radiotherapy modulated tumor hypoxia and increased radiotherapy efficacy, acting to reduce tumor growth, VEGF expression, and vascular density. MDNP treatment also increased apoptosis and DNA double strand breaks, increasing median host survival 3- to 5-fold. Notably, in the murine model, approximately 40% of tumor-bearing mice were tumor-free after a single treatment with MDNPs plus radiotherapy at a 2.5-fold lower dose than required to achieve the same curative treatment without MDNPs. Overall, our findings offer a preclinical proof of concept for the use of MDNP formulations as effective radiotherapy adjuvants.
机译:肿瘤微环境(TME)中的缺氧介导了对放射治疗的抵抗力,并导致接受放射治疗的患者预后不良。在这里,我们报告了使用生物相容性材料通过与内源性H2O2反应使TME复氧的混合二氧化锰(MnO2)纳米颗粒(MDNP)临床上适合的配方设计。含有亲水性三元共聚物-蛋白质-MnO2或疏水性聚合物-脂质-MnO2的MDNP在TME中提供了与不同临床环境相关的不同氧气生成速率。在高度缺氧的小鼠或人类异种移植乳腺肿瘤模型中,我们发现在放疗前施用MDNP制剂可调节肿瘤缺氧并提高放疗功效,从而降低肿瘤生长,VEGF表达和血管密度。 MDNP处理还增加了细胞凋亡和DNA双链断裂,使中位宿主存活率提高了3到5倍。值得注意的是,在鼠模型中,用MDNP加放射疗法单次治疗后,大约40%的荷瘤小鼠是无肿瘤的,剂量要比不使用MDNP进行相同的治疗所需的剂量低2.5倍。总体而言,我们的发现为使用MDNP制剂作为有效的放射治疗佐剂提供了临床前概念证明。

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