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Imaging the delivery of brain-penetrating PLGA nanoparticles in the brain using magnetic resonance

机译:使用磁共振成像对大脑中可穿透大脑的PLGA纳米颗粒的递送进行成像

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摘要

Current therapy for glioblastoma multiforme (GBM) is largely ineffective, with nearly universal tumor recurrence. The failure of current therapy is primarily due to the lack of approaches for the efficient delivery of therapeutics to diffuse tumors in the brain. In our prior study, we developed brain-penetrating nanoparticles that are capable of penetrating brain tissue and distribute over clinically relevant volumes when administered via convection-enhanced delivery (CED). We demonstrated that these particles are capable of efficient delivery of chemotherapeutics to diffuse tumors in the brain, indicating that they may serve as a groundbreaking approach for the treatment of GBM. In the original study, nanoparticles in the brain were imaged using positron emission tomography (PET). However, clinical translation of this delivery platform can be enabled by engineering a non-invasive detection modality using magnetic resonance imaging (MRI). For this purpose, in this study, we developed chemistry to incorporate superparamagnetic iron oxide (SPIO) into the brain-penetrating nanoparticles. We demonstrated that SPIO-loaded nanoparticles, which remain the same morphology as nanoparticles without SPIO, have an excellent transverse (T2) relaxivity. After CED, the distribution of nanoparticles in the brain (i.e., in the vicinity of injection site) can be detected using MRI and the long-lasting signal attenuation of SPIO-loaded brain-penetrating nanoparticles lasted over a one-month timecourse. Development of these nanoparticles is significant as, in future clinical applications, co-administration of SPIO-loaded nanoparticles will allow for intraoperative monitoring of particle distribution in the brain to ensure drug-loaded nanoparticles reach tumors as well for monitoring the therapeutic benefit with time and to evaluate tumor relapse patterns.
机译:目前对多形性胶质母细胞瘤(GBM)的治疗基本上无效,肿瘤复发普遍。当前疗法的失败主要是由于缺乏有效递送疗法以扩散脑部肿瘤的方法。在我们先前的研究中,我们开发了可穿透脑组织的脑穿透纳米颗粒,当通过对流增强递送(CED)给药时,它们能够穿透临床相关体积。我们证明了这些颗粒能够有效地递送化学治疗剂以扩散脑中的肿瘤,表明它们可以作为治疗GBM的突破性方法。在原始研究中,使用正电子发射断层扫描(PET)对大脑中的纳米颗粒成像。但是,可以通过使用磁共振成像(MRI)设计非侵入性检测方式来实现此交付平台的临床翻译。为此,在本研究中,我们开发了将超顺磁性氧化铁(SPIO)掺入可穿透大脑的纳米粒子的化学方法。我们证明了与没有SPIO的纳米粒子保持相同形态的SPIO加载的纳米粒子具有出色的横向(T2)弛豫性。 CED后,可以使用MRI检测纳米颗粒在大脑中的分布(即在注射部位附近),并且SPIO加载的穿透脑的纳米颗粒的信号衰减持续了一个月的时间。这些纳米颗粒的开发意义重大,因为在未来的临床应用中,共同施用SPIO负载的纳米颗粒将可以在术中监测大脑中的颗粒分布,以确保药物负载的纳米颗粒到达肿瘤以及随时间和时间来监测治疗效果。评估肿瘤复发模式。

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