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Forward multiple scattering dominates speckle decorrelation in whole-blood flowmetry using optical coherence tomography

机译:使用光学相干断层扫描在全血流测量中正向多重散射主导斑点去相关

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摘要

Quantitative blood flow measurements using optical coherence tomography (OCT) have a wide potential range of medical research and clinical applications. Flowmetry based on the temporal dynamics of the OCT signal may have the ability to measure three-dimensional flow profiles regardless of the flow direction. State-of-the-art models describing the OCT signal temporal statistics are based on dynamic light scattering (DLS), a model which is inherently limited to single scattering regimes. DLS methods continue to be applied to OCT despite the knowledge that red blood cells produce strong forward multiple scattering. Here, we postulate that forward multiple scattering is the primary mechanism causing the rate of speckle-decorrelation derived from data acquired to deviate from the rate of decorrelation determined in phantom experiments. We also postulate that multiple scattering contributions to decorrelation are only present when the sample exhibits velocity field inhomogeneities larger than the scale of a resolution volume and are thus absent in rigid bulk motion. To test these hypotheses, we performed a systematic study of the effects of forward multiple scattering on OCT signal decorrelation with phantom experiments under physiologically relevant flow conditions and relative bulk motion. Our experimental results confirm that the amount of forward multiple scattering affects the proportionality between lateral flow and decorrelation. We propose that multiply scattered light carries information from different locations in the sample and each location imprints scattering dynamics on the scattered light causing increased decorrelation rates. Our analysis confirms that the detection of forward scattered light inside the vessel lumen causes an increase in the rate of decorrelation which results in an overestimation of blood flow velocities at depths as shallow as 40 µm into whole blood for OCT systems with typical numerical apertures used in retinal imaging.
机译:使用光学相干断层扫描(OCT)进行定量血流测量具有广泛的医学研究和临床应用潜力。基于OCT信号的时间动态的流量分析可能具有测量三维流动曲线的能力,而与流动方向无关。描述OCT信号时间统计信息的最新模型基于动态光散射(DLS),该模型固有地限于单个散射机制。尽管已知红细胞会产生强正向多重散射,但DLS方法仍继续应用于OCT。在这里,我们假定正向多重散射是导致散斑去相关率的主要机制,散斑去相关率从获取的数据中得出,而散斑去相关率却与幻像实验中确定的去相关率背离。我们还假定只有当样品显示出的速度场不均匀性大于解析体积的大小,并且因此在刚体运动中不存在时,才存在对去相关的多重散射贡献。为了检验这些假设,我们使用幻影实验在生理相关的流动条件和相对体积运动下,对正向多重散射对OCT信号去相关的影响进行了系统的研究。我们的实验结果证实,前向多次散射的量会影响横向流动与去相关之间的比例关系。我们提出,散射光的乘积会携带来自样本中不同位置的信息,并且每个位置都会在散射光上施加散射动力学,从而导致去相关率增加。我们的分析证实,检测到血管内腔中的前向散射光会导致去相关速率的增加,从而导致高估了进入全血的OCT系统中使用典型数值孔径的深至40 µm的血流速度。视网膜成像。

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