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System configuration optimization for mesoscopic fluorescence molecular tomography

机译:介观荧光分子层析成像的系统配置优化

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摘要

Tissue engineering applications demand 3D, non-invasive, and longitudinal assessment of bioprinted constructs. Current emphasis is on developing tissue constructs mimicking conditions; however, these are increasingly challenging to image as they are typically a few millimeters thick and turbid, limiting the usefulness of classical fluorescence microscopic techniques. For such applications, we developed a Mesoscopic Fluorescence Molecular Tomography methodology that collects high information content data to enable high-resolution tomographic reconstruction of fluorescence biomarkers at millimeters depths. This imaging approach is based on an inverse problem; hence, its imaging performances are dependent on critical technical considerations including optode sampling, forward model design and inverse solver parameters. Herein, we investigate the impact of the optical system configuration parameters, including detector layout, number of detectors, combination of detector and source numbers, and scanning mode with uncoupled or coupled source and detector array, on the 3D imaging performances. Our results establish that an MFMT system with a 2D detection chain implemented in a de-scanned mode provides the optimal imaging reconstruction performances.
机译:组织工程应用需要对生物打印结构进行3D,无创和纵向评估。目前的重点是开发模仿条件的组织构建物;然而,由于它们通常只有几毫米厚且浑浊,因此对成像的挑战越来越大,限制了经典荧光显微镜技术的实用性。对于此类应用,我们开发了介观荧光分子层析成像方法,该方法可收集大量信息内容数据,以实现毫米深度的荧光生物标记物的高分辨率层析成像重建。这种成像方法是基于反问题的。因此,其成像性能取决于关键技术考虑因素,包括光电采样,正向模型设计和反求解器参数。在本文中,我们调查了光学系统配置参数(包括探测器布局,探测器数量,探测器和光源编号的组合以及具有未耦合或耦合光源和探测器阵列的扫描模式)对3D成像性能的影响。我们的研究结果表明,以反扫描模式实施的带有2D检测链的MFMT系统可提供最佳的成像重建性能。

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