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迈向纳米级乳腺造影对比剂:模块化临床前双光/ X 射线造影剂的开发。

Towards a nanoscale mammographic contrast agent: development of a modular pre-clinical dual optical/x-ray agent.

机构信息

Physical Sciences, Sunnybrook Research Institute, 2075 Bayview Avenue, Toronto, Ontario M4N 3M5, Canada.

出版信息

Phys Med Biol. 2013 Aug 7;58(15):5215-35. doi: 10.1088/0031-9155/58/15/5215. Epub 2013 Jul 12.

Abstract

Contrast-enhanced digital mammography (CEDM) can provide improved breast cancer detection and characterization compared to conventional mammography by imaging the effects of tumour angiogenesis. Current small-molecule contrast agents used for CEDM are limited by a short plasma half-life and rapid extravasation into tissue interstitial space. To address these limitations, nanoscale agents that can remain intravascular except at sites of tumour angiogenesis can be used. For CEDM, this agent must be both biocompatible and strongly attenuate mammographic energy x-rays. Nanoscale perfluorooctylbromide (PFOB) droplets have good x-ray attenuation and have been used in patients for other applications. However, the macroscopic scale of x-ray imaging (50-100 µm) is inadequate for direct verification that PFOB droplets localize at sites of breast tumour angiogenesis. For efficient pre-clinical optimization for CEDM, we integrated an optical marker into PFOB droplets for microscopic assessment (≪50 µm). To develop PFOB droplets as a new nanoscale mammographic contrast agent, PFOB droplets were labelled with fluorescent quantum dots (QDs). The droplets had mean diameters of 160 nm, fluoresced at 635 nm and attenuated x-ray spectra at 30.5 keV mean energy with a relative attenuation of 5.6 ± 0.3 Hounsfield units (HU) mg(-1) mL(-1) QD-PFOB. With the agent loaded into tissue phantoms, good correlation between x-ray attenuation and optical fluorescence was found (R(2) = 0.96), confirming co-localization of the QDs with PFOB for quantitative assessment using x-ray or optical methods. Furthermore, the QDs can be removed from the PFOB agent without affecting its x-ray attenuation or structural properties for expedited translation of optimized PFOB droplet formulations into patients.

摘要

与传统乳腺 X 光相比,对比增强数字乳腺 X 光摄影(CEDM)通过对肿瘤血管生成的影响进行成像,可以提高乳腺癌的检测和特征描述能力。目前用于 CEDM 的小分子对比剂受到血浆半衰期短和快速渗出到组织间质空间的限制。为了解决这些限制,可以使用可以保持在血管内而不是在肿瘤血管生成部位的纳米级试剂。对于 CEDM,该试剂必须既具有生物相容性又能强烈衰减乳腺 X 射线能量。纳米级全氟辛基溴化物(PFOB)液滴具有良好的 X 射线衰减能力,已用于其他应用的患者。然而,X 射线成像的宏观尺度(50-100μm)不足以直接验证 PFOB 液滴是否定位于乳腺肿瘤血管生成部位。为了有效地进行 CEDM 的临床前优化,我们将光学标记物整合到 PFOB 液滴中进行微观评估(≪50μm)。为了将 PFOB 液滴开发为新型纳米级乳腺 X 光造影剂,我们用荧光量子点(QDs)标记了 PFOB 液滴。液滴的平均直径为 160nm,在 635nm 处发荧光,在 30.5keV 平均能量的 X 射线光谱下衰减,相对衰减为 5.6±0.3 亨氏单位(HU)mg-1mL-1QD-PFOB。当将该试剂加载到组织体模中时,发现 X 射线衰减与光学荧光之间存在良好的相关性(R2=0.96),证实了 QD 与 PFOB 的共定位,可用于使用 X 射线或光学方法进行定量评估。此外,QD 可以从 PFOB 试剂中去除而不会影响其 X 射线衰减或结构特性,从而加快优化的 PFOB 液滴制剂向患者的转化。

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