Department of Applied Bioengineering, Graduate School of Convergence Science and Technology, Seoul National University, Seoul, South Korea.
Department of Radiation Oncology, Seoul National University Hospital, Seoul, South Korea.
Med Phys. 2023 Jan;50(1):529-539. doi: 10.1002/mp.16070. Epub 2022 Nov 25.
X-ray fluorescence (XRF) imaging for metal nanoparticles (MNPs) is a promising molecular imaging modality that can determine dynamic biodistributions of MNPs. However, it has the limitation that it only provides functional information.
In this study, we aim to show the feasibility of acquiring functional and anatomic information on the same platform by demonstrating a dual imaging modality of pinhole XRF and computed tomography (CT) for gold nanoparticle (GNP)-injected living mice.
By installing a transmission CT detector in an existing pinhole XRF imaging system using a two-dimensional (2D) cadmium zinc telluride (CZT) gamma camera, XRF and CT images were acquired on the same platform. Due to the optimal X-ray spectra for XRF and CT image acquisition being different, XRF and CT imaging were performed by 140 and 50 kV X-rays, respectively. An amount of 40 mg GNPs (1.9 nm in diameter) suspended in 0.20 ml of phosphate-buffered saline were injected into the three BALB/c mice via a tail vein. Then, the kidney and tumor slices of mice were scanned at specific time points within 60 min to acquire time-lapse in vivo biodistributions of GNPs. XRF images were directly acquired without image reconstruction using a pinhole collimator and a 2D CZT gamma camera. Subsequently, CT images were acquired by performing CT scans. In order to confirm the validity of the functional information provided by the XRF image, the CT image was fused with the XRF image. After the XRF and CT scan, the mice were euthanized, and major organs (kidneys, tumor, liver, and spleen) were extracted. The ex vivo GNP concentrations of the extracted organs were measured by inductively coupled plasma mass spectrometry (ICP-MS) and L-shell XRF detection system using a silicon drift detector, then compared with the in vivo GNP concentrations measured by the pinhole XRF imaging system.
Time-lapse XRF images were directly acquired without rotation and translation of imaging objects within an acquisition time of 2 min per slice. Due to the short image acquisition time, the time-lapse in vivo biodistribution of GNPs was acquired in the organs of the mice. CT images were fused with the XRF images and successfully confirmed the validity of the XRF images. The difference in ex vivo GNP concentrations measured by the L-shell XRF detection system and ICP-MS was 0.0005-0.02% by the weight of gold (wt%). Notably, the in vivo and ex vivo GNP concentrations in the kidneys of three mice were comparable with a difference of 0.01-0.08 wt%.
A dual imaging modality of pinhole XRF and CT imaging system and L-shell XRF detection system were successfully developed. The developed systems are a promising modality for in vivo imaging and ex vivo quantification for preclinical studies using MNPs. In addition, we discussed further improvements for the routine preclinical applications of the systems.
X 射线荧光(XRF)成像技术可用于检测金属纳米粒子(MNPs),是一种很有前途的分子成像方式,可用于测定 MNPs 的动态生物分布。然而,它的局限性在于仅提供功能信息。
本研究旨在展示通过对注射金纳米粒子(GNP)的活体小鼠进行针孔 XRF 和计算机断层扫描(CT)的双重成像模式,在同一平台上获取功能和解剖信息的可行性。
通过在现有的针孔 XRF 成像系统中安装二维(2D)碲化镉锌(CZT)伽马相机作为透射 CT 探测器,在同一平台上获取 XRF 和 CT 图像。由于 XRF 和 CT 图像采集的最佳 X 射线光谱不同,XRF 和 CT 成像分别采用 140 和 50 kV X 射线进行。将 40mg 悬浮在 0.20ml 磷酸盐缓冲盐中的 1.9nm 直径的 GNP 通过尾静脉注入 3 只 BALB/c 小鼠体内。然后,在 60 分钟内的特定时间点扫描小鼠的肾脏和肿瘤切片,以获取 GNP 在体内的时间分辨生物分布。使用针孔准直器和 2D CZT 伽马相机直接采集 XRF 图像,无需图像重建。随后,通过进行 CT 扫描获取 CT 图像。为了确认 XRF 图像提供的功能信息的有效性,将 CT 图像与 XRF 图像融合。在 XRF 和 CT 扫描后,处死小鼠,并提取主要器官(肾脏、肿瘤、肝脏和脾脏)。使用感应耦合等离子体质谱法(ICP-MS)和硅漂移探测器的 L 壳层 XRF 检测系统测量提取器官中的 GNP 浓度,并与通过针孔 XRF 成像系统测量的体内 GNP 浓度进行比较。
在 2 分钟/切片的采集时间内,无需对成像物体进行旋转和移动,即可直接采集时间分辨 XRF 图像。由于图像采集时间短,因此可以在小鼠的器官中获取 GNP 的体内时间分辨生物分布。将 CT 图像与 XRF 图像融合,并成功确认了 XRF 图像的有效性。L 壳层 XRF 检测系统和 ICP-MS 测量的体外 GNP 浓度的差异为金重量的 0.0005-0.02%。值得注意的是,三只小鼠肾脏的体内和体外 GNP 浓度相当,差异为 0.01-0.08 wt%。
成功开发了针孔 XRF 和 CT 成像系统和 L 壳层 XRF 检测系统的双重成像模式。该系统有望成为使用 MNPs 进行体内成像和临床前研究中体外定量的一种有前途的方法。此外,我们还讨论了系统常规临床前应用的进一步改进。
