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PSMA-targeted theranostic nanoplex for prostate cancer therapy

机译:PSMA靶向的治疗纳米复合物用于前列腺癌治疗

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Theranostic imaging, where diagnosis is combined with therapy, is particularly suitable for a disease that is as complex as cancer, especially now that genomic and proteomic profiling can provide an extensive "fingerprint" of each tumor. With such information, theranostic agents can be designed to personalize treatment and minimize damage to normal tissue. Here we have developed a nanoplex platform for theranostic imaging of prostate cancer (PCa). In these proof-of-principle studies, a therapeutic nanoplex containing multimodal imaging reporters was targeted to prostate-specific membrane antigen (PSMA), which is expressed on the cell surface of castrate-resistant PCa. The nanoplex was designed to deliver small interfering RNA (siRNA) along with a prodrug enzyme to PSMA-expressing tumors. Each component of the nanoplex was carefully selected to evaluate its diagnostic aspect of PSMA imaging and its therapeutic aspects of siRNA-mediated down-regulation of a target gene and the conversion of a prodrug to cytotoxic drug, using noninvasive multimodality imaging. Studies performed using two variants of human PC3-PCa cells and tumors, one with high PSMA expression level and another with negligible expression levels, demonstrated PSMA-specific uptake. In addition, down-regulation of the selected siRNA target, choline kinase (Chk), and the conversion of the nontoxic prodrug 5-fluorocytosine (5-FC) to cytotoxic 5-fluorouracil (5-FU) were also demonstrated with noninvasive imaging. The nanoplex was well-tolerated and did not induce liver or kidney toxicity or a significant immune response. The nanoplex platform described can be easily modified and applied to different cancers, receptors, and pathways to achieve theranostic imaging, as a single agent or in combination with other treatment modalities.
机译:诊断和治疗相结合的神经病学成像特别适合于与癌症一样复杂的疾病,尤其是现在,基因组和蛋白质组学分析可以为每种肿瘤提供广泛的“指纹”。有了这样的信息,可以设计治疗治疗剂,以个性化治疗并使对正常组织的损害最小化。在这里,我们已经开发了用于前列腺癌(PCa)肿瘤学成像的nanoplex平台。在这些原理验证研究中,包含多模式成像报告基因的治疗性纳米复合物靶向前列腺特异性膜抗原(PSMA),该抗原在去势抵抗性PCa细胞表面表达。纳米复合体被设计为将小干扰RNA(siRNA)和前药酶一起递送至表达PSMA的肿瘤。使用无创多模态成像技术,精心选择了纳米复合物的每个成分,以评估其PSMA成像的诊断方面以及siRNA介导的靶基因下调的治疗方面以及前药向细胞毒性药物的转化。使用人类PC3-PCa细胞和肿瘤的两种变异进行的研究表明,一种具有较高的PSMA表达水平,而另一种具有可忽略的表达水平,则证明了PSMA特异性摄取。此外,还通过无创成像证实了所选siRNA靶标,胆碱激酶(Chk)的下调以及无毒前药5-氟胞嘧啶(5-FC)向细胞毒性5-氟尿嘧啶(5-FU)的转化。纳米复合物具有良好的耐受性,不会引起肝或肾毒性或明显的免疫反应。所描述的纳米复合物平台可以很容易地进行修饰,并以单一药物或与其他治疗方式结合的方式应用于不同的癌症,受体和途径,以实现治疗诊断成像。

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