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肿瘤的葡萄糖受体磁共振成像:聚乙二醇化顺磁性囊泡对小鼠的研究

Glucose-receptor MR imaging of tumors: study in mice with PEGylated paramagnetic niosomes.

作者信息

Luciani Alain, Olivier Jean-Christophe, Clement Olivier, Siauve Nathalie, Brillet Pierre-Yves, Bessoud Bertrand, Gazeau Florence, Uchegbu Ijeoma F, Kahn Edmond, Frija Guy, Cuenod Charles A

机构信息

Radiology Department, Hôpital Européen Georges Pompidou, INSERM U494, LRI, Faculté Necker, 20 Rue Leblanc, 75015 Paris, France.

出版信息

Radiology. 2004 Apr;231(1):135-42. doi: 10.1148/radiol.2311021559. Epub 2004 Feb 27.

Abstract

PURPOSE

To evaluate a magnetic resonance (MR) imaging contrast agent for tumor detection based on paramagnetic nonionic vesicles (niosomes) bearing polyethylene glycol (PEG) and glucose conjugates for the targeting of overexpressed glucose receptors.

MATERIALS AND METHODS

Four gadobenate dimeglumine-loaded niosome preparations including nonconjugated niosomes, niosomes bearing glucose conjugates (N-palmitoyl glucosamine [NPG]), niosomes bearing PEG 4400, and niosomes bearing both PEG and NPG were tested. In vitro cellular uptake was measured at electron paramagnetic resonance (EPR) after incubation with human prostate carcinoma, PC3, cells. In vivo distribution was studied at MR imaging 6, 12, and 24 hours after injection, with assessment of tumor, brain, liver, and muscle signal intensity (SI) in 49 mice bearing PC3 cells. Efficiency of targeted contrast agents was assessed with tumor-to-muscle contrast-to-noise ratio (CNR). Testing for differences was performed with analysis of variance followed by a posteriori Fisher test.

RESULTS

In vitro, gadolinium could be detected at EPR only in cell pellets incubated with niosomes bearing glucose conjugates or niosomes bearing both glucose conjugates and PEG (4.9. 10(-15) and 4.5. 10(-15) mol gadolinium per PC3 cell). In vivo, marked predominant tumor enhancement was demonstrated 24 hours after injection of glycosylated PEG niosomes (P <.01); no significant differences were observed following injection of nonconjugated niosomes, glycosylated niosomes, or PEG 4400 niosomes. Twenty-four hours after injection, sole presence of NPG or PEG 4400 on the surface of the niosome led to higher tumor-to-muscle CNR than that observed after injection of nonconjugated niosomes (CNR of 3.3 +/- 0.7 [SD], 3.4 +/- 2.2, and 0 +/- 1.9). Combination of NPG and PEG led to even higher tumor-to-muscle CNR (6.3 +/- 2.2).

CONCLUSION

Combination of PEG and glucose conjugates on the surface of niosomes significantly improved tumor targeting of an encapsulated paramagnetic agent assessed with MR imaging in a human carcinoma xenograft model.

摘要

目的

评估一种基于携带聚乙二醇(PEG)和葡萄糖共轭物的顺磁性非离子囊泡(脂质体)的磁共振(MR)成像造影剂,用于靶向过表达的葡萄糖受体以检测肿瘤。

材料与方法

测试了四种载有钆布醇的脂质体制剂,包括未共轭的脂质体、携带葡萄糖共轭物的脂质体(N-棕榈酰葡糖胺 [NPG])、携带PEG 4400的脂质体以及同时携带PEG和NPG的脂质体。与人前列腺癌PC3细胞孵育后,通过电子顺磁共振(EPR)测量体外细胞摄取情况。在注射后6、12和24小时进行MR成像研究体内分布,评估49只携带PC3细胞的小鼠的肿瘤、脑、肝和肌肉信号强度(SI)。用肿瘤与肌肉的对比噪声比(CNR)评估靶向造影剂的效率。采用方差分析及事后Fisher检验进行差异检验。

结果

体外,仅在与携带葡萄糖共轭物的脂质体或同时携带葡萄糖共轭物和PEG的脂质体孵育的细胞沉淀中,通过EPR能检测到钆(每个PC3细胞中钆的含量分别为4.9×10⁻¹⁵和4.5×10⁻¹⁵摩尔)。体内,注射糖基化PEG脂质体后24小时显示出明显的肿瘤显著强化(P <.01);注射未共轭脂质体组、糖基化脂质体组或PEG 4400脂质体组后未观察到显著差异。注射后24小时,脂质体表面仅存在NPG或PEG 4400时,肿瘤与肌肉的CNR高于注射未共轭脂质体后的情况(CNR分别为3.3±0.7 [标准差]、3.4±2.2和0±1.9)。NPG和PEG的组合使肿瘤与肌肉的CNR更高(6.3±2.2)。

结论

在人癌异种移植模型中,脂质体表面PEG与葡萄糖共轭物的组合显著改善了用MR成像评估的包封顺磁性剂的肿瘤靶向性。

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