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体内单乳腺癌微钙化的高分辨率计算机断层扫描。

High-resolution computed tomography of single breast cancer microcalcifications in vivo.

机构信息

Division of Hematology/Oncology and Department of Radiology, Beth Israel Deaconess Medical Center, Boston, MA 02215, USA.

出版信息

Mol Imaging. 2011 Aug;10(4):295-304. doi: 10.2310/7290.2010.00050. Epub 2011 Apr 1.

Abstract

Microcalcification is a hallmark of breast cancer and a key diagnostic feature for mammography. We recently described the first robust animal model of breast cancer microcalcification. In this study, we hypothesized that high-resolution computed tomography (CT) could potentially detect the genesis of a single microcalcification in vivo and quantify its growth over time. Using a commercial CT scanner, we systematically optimized acquisition and reconstruction parameters. Two ray-tracing image reconstruction algorithms were tested: a voxel-driven "fast" cone beam algorithm (FCBA) and a detector-driven "exact" cone beam algorithm (ECBA). By optimizing acquisition and reconstruction parameters, we were able to achieve a resolution of 104 μm full width at half-maximum (FWHM). At an optimal detector sampling frequency, the ECBA provided a 28 μm (21%) FWHM improvement in resolution over the FCBA. In vitro, we were able to image a single 300 μm × 100 μm hydroxyapatite crystal. In a syngeneic rat model of breast cancer, we were able to detect the genesis of a single microcalcification in vivo and follow its growth longitudinally over weeks. Taken together, this study provides an in vivo "gold standard" for the development of calcification-specific contrast agents and a model system for studying the mechanism of breast cancer microcalcification.

摘要

微钙化是乳腺癌的一个标志,也是乳房 X 线照相术的一个关键诊断特征。我们最近描述了第一个稳健的乳腺癌微钙化动物模型。在这项研究中,我们假设高分辨率计算机断层扫描(CT)有可能在体内检测到单个微钙化的发生,并随时间定量其生长。我们使用商业 CT 扫描仪系统地优化了采集和重建参数。测试了两种射线追踪图像重建算法:一种是体素驱动的“快速”锥形束算法(FCBA)和一种是探测器驱动的“精确”锥形束算法(ECBA)。通过优化采集和重建参数,我们能够实现 104μm 的分辨率(半最大值全宽,FWHM)。在最佳探测器采样频率下,ECBA 相对于 FCBA 在分辨率方面提供了 28μm(21%)的改善。在体外,我们能够对单个 300μm×100μm 的羟磷灰石晶体进行成像。在乳腺癌的同基因大鼠模型中,我们能够在体内检测到单个微钙化的发生,并在数周内对其生长进行纵向跟踪。总之,这项研究为钙化特异性对比剂的开发提供了体内“金标准”,并为研究乳腺癌微钙化的机制提供了模型系统。

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