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Enhancement of HIFU ablation by sonosensitizer-loading liquid fluorocarbon nanoparticles with pre-targeting in a mouse model

机译:通过在小鼠模型中预靶向声敏剂加载液态碳氟化合物纳米颗粒增强HIFU消融

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摘要

High intensity focused ultrasound (HIFU) is a noninvasive thermal ablation technique for the treatment of benign and malignant solid masses. To improve the efficacy of HIFU ablation, we developed poly (lactide-co-glycolide) (PLGA) nanoparticles encapsulating perfluoropentane (PFP) and hematoporphyrin monomethyl ether (HMME) as synergistic agents (HMME+PFP/PLGA). Two-step biotin-avidin pre-targeting technique was applied for the HIFU ablation. We further modified the nanoparticles with streptavidin (HMME+PFP/PLGA-SA). HMME+PFP/PLGA-SA were highly dispersed with spherical morphology (477.8 ± 81.8 nm in diameter). The encapsulation efficiency of HMME and PFP were 46.6 ± 3.3% and 40.1 ± 2.6%, respectively. The binding efficiency of nanoparticles to streptavidin was 95.5 ± 2.5%. The targeting ability of the HMME+PFP/PLGA-SA nanoparticles was tested by parallel plate flow chamber in vitro. In the pre-targeting group (HMME+PFP/PLGA-SA), a large number of nanoparticles bound to the peripheral and surface of the cell. In the HIFU ablation experiment in vivo, compared with the other groups, the largest gray-scale changes and coagulation necrosis areas were observed in the pre-targeting (HMME+PFP/PLGA-SA) group, with the lowest energy efficiency factor value. Moreover, the microvessel density and proliferation index declined, while the apoptotic index increased, in the tumor tissue surrounding the coagulation necrosis area in the pre-targeting group. Meanwhile, the survival time of the tumor-bearing nude mice in the pre-targeting group was significantly longer than that in the HIFU treatment group. These results suggest that HMME+PFP/PLGA-SA have high potential to act as synergistic agents in HIFU ablation.
机译:高强度聚焦超声(HIFU)是一种用于治疗良性和恶性固体肿块的无创热消融技术。为了提高HIFU消融的疗效,我们开发了聚全丙交酯(PFP)和血卟啉单甲醚(HMME)作为增效剂(HMME + PFP / PLGA)的聚丙交酯-乙交酯共聚物(PLGA)。采用两步生物素-亲和素预靶向技术进行HIFU消融。我们用链霉亲和素(HMME + PFP / PLGA-SA)进一步修饰了纳米颗粒。 HMME + PFP / PLGA-SA高度分散,呈球形(直径477.8±81.8nm)。 HMME和PFP的包封效率分别为46.6±3.3%和40.1±2.6%。纳米粒子与链霉亲和素的结合效率为95.5±2.5%。 HMME + PFP / PLGA-SA纳米粒子的靶向能力在体外通过平行板流动室测试。在预靶向组(HMME + PFP / PLGA-SA)中,大量纳米颗粒结合到细胞的外围和表面。在体内HIFU消融实验中,与其他组相比,在预靶向(HMME + PFP / PLGA-SA)组中观察到最大的灰度变化和凝血坏死区域,能量效率因子值最低。此外,在预靶向组中,在凝血坏死区域周围的肿瘤组织中,微血管密度和增殖指数下降,而凋亡指数上升。同时,预靶向组的荷瘤裸鼠的生存时间明显长于HIFU治疗组。这些结果表明,HMME + PFP / PLGA-SA在HIFU消融中具有协同作用的潜力。

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