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用于区分癌症与良性软组织的新型大分子聚合磁共振成像造影剂。

New macromolecular polymeric MRI contrast agents for application in the differentiation of cancer from benign soft tissues.

作者信息

Cyran Clemens C, Fu Yanjun, Raatschen Hans-Juergen, Rogut Victor, Chaopathomkul Bundit, Shames David M, Wendland Michael F, Yeh Benjamin M, Brasch Robert C

机构信息

Center for Pharmaceutical and Molecular Imaging, Department of Radiology, University of California San Francisco, San Francisco, CA 94143-0628, USA.

出版信息

J Magn Reson Imaging. 2008 Mar;27(3):581-9. doi: 10.1002/jmri.21245.

Abstract

PURPOSE

To compare three new macromolecular polyethylene glycol (PEG) -core dendrimeric gadolinium(Gd)-based MRI contrast agents for their applicability in quantitative assays of endothelial leakiness and tissue vascular density for the differentiation of cancer from normal soft tissues.

MATERIALS AND METHODS

Thirty-two athymic rats with human breast cancer xenografts (MDA-MB-435) were imaged by dynamic MRI following enhancement with one of three new (Gd-DOTA)-conjugated PEG-core dendrimer contrast agents (effective molecular weights 161 to 323 kDa). Results were compared with a prototype macromolecular contrast agent, albumin (Gd-DTPA). Assays of permeabilities (K(PS); microL/min . 100 cm(3)) and tumor fractional plasma volumes (%) based on a two-compartment kinetic model were performed for skeletal muscle and tumors.

RESULTS

The largest PEG-core contrast agent, PEG(20,000)-Gen4-(Gd-DOTA), leaked in breast tumors (K(PS) = 50 +/- 23 microL/min . 100 cm(3)), while exhibiting no measurable transendothelial leak (K(PS) = 0 microL/min . 100 cm(3)) in normal soft tissue microvessels allowing successful differentiation (P < 0.05) of cancers from normal muscle. PEG(12,000)-Gen4-(Gd-DOTA) leaked in tumors and in normal muscle (K(PS) = 51 +/- 26 and K(PS) = 21 +/- 18 microL/min . 100 cm(3), respectively). The smallest agent, PEG(12,000)-Gen3-(Gd-DOTA) also showed a measurable leak in both normal and malignant microvessels.

CONCLUSION

MRI assays of vascular endothelial leakiness using new PEG-core, (Gd-DOTA)-conjugated macromolecular contrast agents proved applicable for the differentiation of human breast cancer from normal soft tissue. The apparent threshold in effective molecular weight for a clear differentiation of cancer from normal muscle with no measurable leak in the muscle is between 194 and 323 kDa.

摘要

目的

比较三种新型基于大分子聚乙二醇(PEG)核心的钆(Gd)磁共振成像(MRI)造影剂,评估其在定量检测内皮渗漏及组织血管密度以鉴别癌症与正常软组织方面的适用性。

材料与方法

32只接种人乳腺癌异种移植物(MDA-MB-435)的无胸腺大鼠,在注射三种新型(钆-二乙三胺五乙酸)共轭PEG核心树枝状造影剂(有效分子量161至323 kDa)之一后进行动态MRI成像。将结果与一种大分子造影剂原型白蛋白(钆-二乙烯三胺五乙酸)进行比较。基于双室动力学模型对骨骼肌和肿瘤进行通透性(K(PS);微升/分钟·100立方厘米)和肿瘤血浆分数体积(%)的检测。

结果

最大的PEG核心造影剂PEG(20,000)-Gen4-(钆-二乙三胺五乙酸)在乳腺肿瘤中渗漏(K(PS)=50±23微升/分钟·100立方厘米),而在正常软组织微血管中无明显的跨内皮渗漏(K(PS)=0微升/分钟·100立方厘米),从而能够成功区分(P<0.05)癌症与正常肌肉。PEG(12,000)-Gen4-(钆-二乙三胺五乙酸)在肿瘤和正常肌肉中均有渗漏(分别为K(PS)=51±26和K(PS)=21±18微升/分钟·100立方厘米)。最小的造影剂PEG(12,000)-Gen3-(钆-二乙三胺五乙酸)在正常和恶性微血管中均有明显渗漏。

结论

使用新型PEG核心、(钆-二乙三胺五乙酸)共轭大分子造影剂进行MRI血管内皮渗漏检测,被证明可用于鉴别人类乳腺癌与正常软组织。有效分子量在19(此处原文可能有误,推测应为194)至323 kDa之间时,能清晰区分癌症与正常肌肉,且肌肉中无明显渗漏。

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