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The Global Burden of Cancer 2013.《2013 年全球癌症负担》。
JAMA Oncol. 2015 Jul;1(4):505-27. doi: 10.1001/jamaoncol.2015.0735.
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J Control Release. 2015 Sep 10;213:79-85. doi: 10.1016/j.jconrel.2015.06.030. Epub 2015 Jun 29.
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Gene therapy for cancer: present status and future perspective.癌症的基因治疗:现状与未来展望。
Mol Cell Ther. 2014 Sep 10;2:27. doi: 10.1186/2052-8426-2-27. eCollection 2014.
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Nanotherapy for Cancer: Targeting and Multifunctionality in the Future of Cancer Therapies.癌症的纳米疗法:癌症治疗未来的靶向性与多功能性
ACS Biomater Sci Eng. 2015 Feb 9;1(2):64-78. doi: 10.1021/ab500084g. Epub 2015 Jan 13.
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Nucleic Acid Therapeutics Using Polyplexes: A Journey of 50 Years (and Beyond).使用多聚体的核酸疗法:50年(及以后)的历程
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cMET in NSCLC: Can We Cut off the Head of the Hydra? From the Pathway to the Resistance.cMET在非小细胞肺癌中的作用:我们能斩断九头蛇的头吗?从信号通路到耐药性
Cancers (Basel). 2015 Mar 25;7(2):556-73. doi: 10.3390/cancers7020556.
8
Mesenchymal stem cell-mediated, tumor stroma-targeted radioiodine therapy of metastatic colon cancer using the sodium iodide symporter as theranostic gene.间充质干细胞介导的、以肿瘤基质为靶点的转移性结肠癌放射性碘治疗,使用碘化钠同向转运体作为诊疗基因。
J Nucl Med. 2015 Apr;56(4):600-6. doi: 10.2967/jnumed.114.146662. Epub 2015 Mar 5.
9
Histidine-rich stabilized polyplexes for cMet-directed tumor-targeted gene transfer.用于cMet导向的肿瘤靶向基因转移的富含组氨酸的稳定多聚体
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10
Defined polymeric materials for gene delivery.用于基因递送的特定聚合材料。
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序列定义的靶向cMET/HGFR的聚合物作为治疗诊断用碘化钠转运体(NIS)基因的基因递送载体。

Sequence-defined cMET/HGFR-targeted Polymers as Gene Delivery Vehicles for the Theranostic Sodium Iodide Symporter (NIS) Gene.

作者信息

Urnauer Sarah, Morys Stephan, Krhac Levacic Ana, Müller Andrea M, Schug Christina, Schmohl Kathrin A, Schwenk Nathalie, Zach Christian, Carlsen Janette, Bartenstein Peter, Wagner Ernst, Spitzweg Christine

机构信息

Department of Internal Medicine II, LMU Munich, Munich, Germany.

Department of Pharmacy, Center of Drug Research, Pharmaceutical Biotechnology, LMU Munich, Munich, Germany.

出版信息

Mol Ther. 2016 Aug;24(8):1395-404. doi: 10.1038/mt.2016.95. Epub 2016 May 9.

DOI:10.1038/mt.2016.95
PMID:27157666
原文链接:https://pmc.ncbi.nlm.nih.gov/articles/PMC5023389/
Abstract

The sodium iodide symporter (NIS) as well-characterized theranostic gene represents an outstanding tool to target different cancer types allowing noninvasive imaging of functional NIS expression and therapeutic radioiodide application. Based on its overexpression on the surface of most cancer types, the cMET/hepatocyte growth factor receptor serves as ideal target for tumor-selective gene delivery. Sequence-defined polymers as nonviral gene delivery vehicles comprising polyethylene glycol (PEG) and cationic (oligoethanoamino) amide cores coupled with a cMET-binding peptide (cMBP2) were complexed with NIS-DNA and tested for receptor-specificity, transduction efficiency, and therapeutic efficacy in hepatocellular cancer cells HuH7. In vitro iodide uptake studies demonstrated high transduction efficiency and cMET-specificity of NIS-encoding polyplexes (cMBP2-PEG-Stp/NIS) compared to polyplexes without targeting ligand (Ala-PEG-Stp/NIS) and without coding DNA (cMBP2-PEG-Stp/Antisense-NIS). Tumor recruitment and vector biodistribution were investigated in vivo in a subcutaneous xenograft mouse model showing high tumor-selective iodide accumulation in cMBP2-PEG-Stp/NIS-treated mice (6.6 ± 1.6% ID/g (123)I, biological half-life 3 hours) by (123)I-scintigraphy. Therapy studies with three cycles of polyplexes and (131)I application resulted in significant delay in tumor growth and prolonged survival. These data demonstrate the enormous potential of cMET-targeted sequence-defined polymers combined with the unique theranostic function of NIS allowing for optimized transfection efficiency while eliminating toxicity.

摘要

碘化钠同向转运体(NIS)作为一种特征明确的诊疗基因,是靶向不同癌症类型的出色工具,可实现功能性NIS表达的无创成像及放射性碘治疗应用。基于其在大多数癌症类型表面的过表达,cMET/肝细胞生长因子受体可作为肿瘤选择性基因递送的理想靶点。将包含聚乙二醇(PEG)和与cMET结合肽(cMBP2)偶联的阳离子(寡乙氨基)酰胺核心的序列定义聚合物作为非病毒基因递送载体,与NIS-DNA复合,并在肝癌细胞HuH7中测试其受体特异性、转导效率和治疗效果。体外碘摄取研究表明,与无靶向配体的聚合物(Ala-PEG-Stp/NIS)和无编码DNA的聚合物(cMBP2-PEG-Stp/反义-NIS)相比,编码NIS的多聚体(cMBP2-PEG-Stp/NIS)具有高转导效率和cMET特异性。在皮下异种移植小鼠模型中对体内肿瘤募集和载体生物分布进行了研究,通过(123)I闪烁扫描显示,在接受cMBP2-PEG-Stp/NIS治疗的小鼠中肿瘤选择性碘积累较高(6.6±1.6%ID/g(123)I,生物半衰期3小时)。用三个周期的多聚体和(131)I进行治疗研究,结果显示肿瘤生长显著延迟,生存期延长。这些数据证明了cMET靶向的序列定义聚合物与NIS独特的诊疗功能相结合的巨大潜力,可实现优化的转染效率同时消除毒性。