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Evaluation of a PSMA-targeted BNF nanoparticle construct

机译:评价一个PSMA-targeted BNF纳米颗粒构造

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Early detection enables improved prognosis for prostate cancer (PCa). A promising target for imaging and therapy of PCa is the prostate-specific membrane antigen (PSMA), which exhibits both expression within the epithelium of PCa cells, and becomes internalized upon ligand binding. Here we report the synthesis of a PSMA-targeted bionized nanoferrite (BNF) nanoparticle and its biological evaluation in an experimental model of PCa. The BNF nanoparticle formulation exhibits properties conducive to targeted imaging such as stealth, prolonged circulation time and enhanced clearance from non-target sites. Optical imaging of the targeted BNF in vivo indicates preferential accumulation in PSMA+ tumors 4 h post-injection, suggesting target specificity. On the other hand, non-targeted nanoparticles exhibit lower uptake with similar accumulation in both PSMA+ and PSMA-tumors indicating tumor access without preferential accumulation. Imaging with single photon emission computed tomography (SPECT) and bio-distribution studies of a modified construct indicate highest tumor accumulation at 48 h post-injection [4.3 +/- 0.4 percentage injected dose per gram of tissue (% ID g(-1))], with tumor/blood and tumor/muscle ratios of 7.5 +/- 2.4 and 11.6 +/- 1.2 % ID g(-1), respectively. Ex vivo fluorescence microscopy, Prussian blue staining, immunohistochemistry and biodistribution studies confirm enhanced nanoparticle uptake in PSMA+ tumors compared to those not expressing PSMA. The BNF nano-formulation described is promising for PSMA-targeted imaging applications in vivo.
机译:早期发现可以改善预后前列腺癌(PCa)。PCa的成像和治疗前列腺特异性膜抗原(PSMA)展品的上皮细胞内表达PCa细胞,成为内化在配体绑定。PSMA-targeted bionized nanoferrite (BNF)纳米颗粒和生物评价的实验的主成分分析模型。有利于制定展览属性目标成像等隐形,延长了循环时间和增强的间隙非目标网站。BNF体内显示优惠积累在+肿瘤4 h post-injection PSMA,建议目标专一性。一道纳米粒子表现出较低的吸收具有类似PSMA +和积累PSMA-tumors表明肿瘤没有访问优惠积累。光子发射计算机断层扫描(SPECT)和生物分布的研究修改后的构造显示最高的肿瘤积累在48 hpost-injection[4.3 + / - 0.4比例注入每克组织剂量(% ID g (1)))肿瘤/血液和肿瘤/肌肉比率为7.5 + / -2.4和11.6 + / - 1.2% ID g(1),分别。活体荧光显微镜,普鲁士蓝染色、免疫组织化学和biodistribution研究证实了纳米颗粒的吸收在PSMA +肿瘤相比那些没有表达PSMA。nano-formulation描述是有前途的PSMA-targeted体内成像应用。

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