利用超声定位显微镜优化临床微血管成像的体内数据采集。

ArXiv Pub Date : 2024-12-24
Chengwu Huang, U-Wai Lok, Jingke Zhang, Xiang Yang Zhu, James D Krier, Amy Stern, Kate M Knoll, Kendra E Petersen, Kathryn A Robinson, Gina K Hesley, Andrew J Bentall, Thomas D Atwell, Andrew D Rule, Lilach O Lerman, Shigao Chen
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摘要

超声定位显微镜(ULM)使微血管成像的空间分辨率超过声衍射极限,具有重要的临床潜力。然而,ULM的性能在很大程度上依赖于微泡(MB)信号的稀疏度、检测到的MB的数量和信噪比(SNR),所有这些在临床情况下都是不同的。这些变化的来源强调了优化MB剂量、数据采集时间和成像设置的必要性,以便标准化和优化微血管ULM。为了优化临床ULM的数据采集,本初步研究在猪和人类模型中研究了大剂量注射期间MB信号的时间变化。开发了量化指标来评估MB信号质量,指导选择采集时间,以平衡MB定位质量和足够的MB计数。并探讨了传输电压和剂量的影响。在猪模型中,在快速冲洗阶段确定了相对较短的最佳采集窗口(约10秒),这突出了在数据采集过程中对实时MB信号监测的需求。人类较慢的冲洗阶段允许1-2分钟的更灵活的成像窗口,同时在不同的冲洗阶段时间观察到定位质量和MB密度(或采集长度)之间的权衡。在这些发现的指导下,利用短时间的数据采集,在猪和人的肾脏中实现了强大的ULM成像,证明了其在临床实践中的可行性。该研究为优化一致性和可重复性ULM的数据采集提供了见解,为其标准化和更广泛的临床应用铺平了道路。
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Optimizing In Vivo Data Acquisition for Robust Clinical Microvascular Imaging Using Ultrasound Localization Microscopy.

Ultrasound localization microscopy (ULM) enables microvascular imaging at spatial resolutions beyond the acoustic diffraction limit, offering significant clinical potentials. However, ULM performance relies heavily on microbubble (MB) signal sparsity, the number of detected MBs, and signal-to-noise ratio (SNR), all of which vary in clinical scenarios involving bolus MB injections. These sources of variations underscore the need to optimize MB dosage, data acquisition timing, and imaging settings in order to standardize and optimize ULM of microvasculature. This pilot study investigated temporal changes in MB signals during bolus injections in both pig and human models to optimize data acquisition for clinical ULM. Quantitative indices were developed to evaluate MB signal quality, guiding selection of acquisition timing that balances the MB localization quality and adequate MB counts. The effects of transmitted voltage and dosage were also explored. In the pig model, a relatively short window (approximately 10 seconds) for optimal acquisition was identified during the rapid wash-out phase, highlighting the need for real-time MB signal monitoring during data acquisition. The slower wash-out phase in humans allowed for a more flexible imaging window of 1-2 minutes, while trade-offs were observed between localization quality and MB density (or acquisition length) at different wash-out phase timings. Guided by these findings, robust ULM imaging was achieved in both pig and human kidneys using a short period of data acquisition, demonstrating its feasibility in clinical practice. This study provides insights into optimizing data acquisition for consistent and reproducible ULM, paving the way for its standardization and broader clinical applications.

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