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Roles of Nanoparticles during Magnetic Resonance Navigation and Bacterial Propulsion for Enhanced Drug Delivery in Tumors

机译:磁共振导航过程中纳米颗粒的作用及肿瘤增强药物递送的细菌推进

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It is well known that the uses of nanoparticles (NPs) can enhance medical imaging, diagnostics, and drug delivery. But for these applications and for drug delivery in particular, the difficulty in targeting specific organs in the body limits the role of these NPs for medical interventions. In cancer therapy for instance, systemic injections of drug-loaded nanoparticles result into an increase of toxicity in the body coupled with a reduction of the therapeutic outcome due to a lack of efficient targeting. Therefore, although the small size of drug-loaded NPs allows them to preferentially accumulate at tumor sites because tumors lack an effective lymphatic drainage system, most of the NPs may not reach the tumor sites but would rather reach healthy organs through systemic circulations. Hence, the challenge would be to deliver the higher percentage of the drug close enough to the tumor sites while avoiding systemic circulations. This can be achieved by adding an additional capability known as Magnetic Resonance Navigation (MRN) to the NPs without compromising their potentials for medical imaging, diagnostics, and drug delivery. MRN used for targeted drug delivery relies on magnetic nanoparticles (MNPs) embedded in therapeutic magnetic microcarriers (TMMCs) where such MNPs being fully saturated in a high homogeneous magnetic field, allow the induction of a pulling force through the use of 3D directional gradients for vascular navigation along a pre-planned path. Although the effectiveness of MRN is independent of the depth at which it operates unlike the use of an external magnet, travel is limited to larger diameter blood vessels. As such, MRN is complemented by bacterial propulsion where drug-loaded MC-1 magnetotactic bacteria (MTB) relying on a chain of NPs known as magnetosomes for directional control and previously transported through MR-compatible microcarriers, are being considered as vehicles capable of reaching the tumor sites through the microvasculature.
机译:众所周知,纳米颗粒(NPS)的用途可以增强医学成像,诊断和药物递送。但对于这些应用和药物递送,特别是靶向体内特定器官的困难限制了这些NPS对医疗干预的作用。例如,在癌症疗法中,由于缺乏有效的靶向,可以增加药物纳米颗粒的系统注射导致体内的毒性增加,其含量减少治疗结果。因此,尽管较小的药物负载的NPS允许它们优先在肿瘤部位积累,因为肿瘤缺乏有效的淋巴引流系统,但大多数NPS可能无法到达肿瘤部位,而是通过系统循环达到健康的器官。因此,挑战是将较高百分比的药物缩短到肿瘤部位,同时避免系统循环。这可以通过将称为磁共振导航(MRN)的额外能力添加到NPS来实现,而不会影响其用于医学成像,诊断和药物递送的潜力。用于靶向药物递送的MRN依赖于嵌入治疗性磁性微载体(TMMC)的磁性纳米颗粒(MNP),其中这种MNP在高均匀的磁场中完全饱和,允许通过使用3D定向梯度来诱导拉动力的血管沿预先计划的路径导航。虽然MRN的有效性与其不同于使用外部磁铁的深度无关,但是行程仅限于较大直径的血管。这样,MRN被细菌推进辅酶互补,其中依赖于称为磁体的NP链的药物负载的MC-1磁体细菌(MTB)被认为是能够到达的车辆被视为车辆的磁性载体肿瘤部位通过微血管。

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