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The effect of nanoparticle polyethylene glycol surface density on ligand-directed tumor targeting studied in vivo by dual modality imaging.通过双模式成像研究纳米粒子聚乙二醇表面密度对配体导向肿瘤靶向的体内影响。
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Imaging vascular function for early stage clinical trials using dynamic contrast-enhanced magnetic resonance imaging.使用动态对比增强磁共振成像进行早期临床试验的血管功能成像。
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Combining antiangiogenics to overcome resistance: rationale and clinical experience.联合抗血管生成药物克服耐药性:原理与临床经验。
Clin Cancer Res. 2012 Jul 15;18(14):3750-61. doi: 10.1158/1078-0432.CCR-11-1275. Epub 2012 Apr 30.
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Anti-angiogenesis therapy in cancer: current challenges and future perspectives.癌症的抗血管生成治疗:当前的挑战与未来展望。
Cancer Lett. 2012 Jul 28;320(2):130-7. doi: 10.1016/j.canlet.2012.03.008. Epub 2012 Mar 13.
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Imaging in the age of molecular medicine: monitoring of anti-angiogenic treatments.分子医学时代的影像学:抗血管生成治疗的监测。
Curr Pharm Biotechnol. 2012 Mar;13(4):595-608. doi: 10.2174/138920112799436348.
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Investigation of In Vivo Targeting Kinetics of α(v)β(3)-Specific Superparamagnetic Nanoprobes by Time-Resolved MRI.采用时间分辨 MRI 研究 α(v)β(3)-特异性超顺磁纳米探针的体内靶向动力学。
Theranostics. 2011 Apr 24;1:263-73. doi: 10.7150/thno/v01p0263.
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Multifunctional nanoemulsion platform for imaging guided therapy evaluated in experimental cancer.多功能纳米乳液平台用于实验性癌症的成像引导治疗评估。
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Nat Rev Clin Oncol. 2011 Mar 1;8(4):210-21. doi: 10.1038/nrclinonc.2011.21.
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The promise of dynamic contrast-enhanced imaging in radiation therapy.动态对比增强成像在放射治疗中的应用前景。
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VEGF-PET imaging is a noninvasive biomarker showing differential changes in the tumor during sunitinib treatment.VEGF-PET 成像技术是一种无创生物标志物,可显示舒尼替尼治疗期间肿瘤的差异变化。
Cancer Res. 2011 Jan 1;71(1):143-53. doi: 10.1158/0008-5472.CAN-10-1088. Epub 2010 Nov 17.

通过纳米颗粒辅助磁共振和近红外荧光分子成像进行肿瘤血管生成表型分析。

Tumor angiogenesis phenotyping by nanoparticle-facilitated magnetic resonance and near-infrared fluorescence molecular imaging.

机构信息

Translational and Molecular Imaging Institute, Mount Sinai School of Medicine, New York, NY 10029, USA.

出版信息

Neoplasia. 2012 Oct;14(10):964-73. doi: 10.1593/neo.121148.

DOI:10.1593/neo.121148
PMID:23097630
原文链接:https://pmc.ncbi.nlm.nih.gov/articles/PMC3479840/
Abstract

One of the challenges of tailored antiangiogenic therapy is the ability to adequately monitor the angiogenic activity of a malignancy in response to treatment. The α(v)β(3) integrin, highly overexpressed on newly formed tumor vessels, has been successfully used as a target for Arg-Gly-Asp (RGD)-functionalized nanoparticle contrast agents. In the present study, an RGD-functionalized nanocarrier was used to image ongoing angiogenesis in two different xenograft tumor models with varying intensities of angiogenesis (LS174T > EW7). To that end, iron oxide nanocrystals were included in the core of the nanoparticles to provide contrast for T(2)*-weighted magnetic resonance imaging (MRI), whereas the fluorophore Cy7 was attached to the surface to enable near-infrared fluorescence (NIRF) imaging. The mouse tumor models were used to test the potential of the nanoparticle probe in combination with dual modality imaging for in vivo detection of tumor angiogenesis. Pre-contrast and post-contrast images (4 hours) were acquired at a 9.4-T MRI system and revealed significant differences in the nanoparticle accumulation patterns between the two tumor models. In the case of the highly vascularized LS174T tumors, the accumulation was more confined to the periphery of the tumors, where angiogenesis is predominantly occurring. NIRF imaging revealed significant differences in accumulation kinetics between the models. In conclusion, this technology can serve as an in vivo biomarker for antiangiogenesis treatment and angiogenesis phenotyping.

摘要

靶向抗血管生成治疗的挑战之一是能够充分监测恶性肿瘤对治疗的血管生成活性。α(v)β(3)整联蛋白在新形成的肿瘤血管中高度过表达,已成功用作 Arg-Gly-Asp(RGD)功能化纳米颗粒对比剂的靶标。在本研究中,使用 RGD 功能化纳米载体在两种不同的异种移植肿瘤模型中成像正在进行的血管生成,这两种模型的血管生成强度不同(LS174T>EW7)。为此,将氧化铁纳米晶体包含在纳米颗粒的核心中,以提供 T(2)*加权磁共振成像(MRI)的对比,而将荧光团 Cy7 附着在表面上以实现近红外荧光(NIRF)成像。使用小鼠肿瘤模型测试纳米颗粒探针与双模态成像相结合在体内检测肿瘤血管生成的潜力。在 9.4-T MRI 系统上采集预对比和对比后(4 小时)图像,并揭示了两种肿瘤模型之间纳米颗粒积累模式的显着差异。在高度血管化的 LS174T 肿瘤中,积累更局限于血管生成主要发生的肿瘤外围。NIRF 成像揭示了模型之间积累动力学的显着差异。总之,该技术可用作抗血管生成治疗和血管生成表型的体内生物标志物。