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Multiple-fiber probe design for fluorescence spectroscopy in tissue

机译:用于组织中荧光光谱的多纤维探针设计

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摘要

The fiber-optic probe is an essential component of many quantitative fluorescence spectroscopy systems, enabling delivery of excitation light and collection of remitted fluorescence in a wide variety of clinical and laboratory situations. However, there is little information available on the role of illumination-collection geometry to guide the design of these components. Therefore we used a Monte Carlo model to investigate the effect of multifiber probe design parameters—numerical aperture, fiber diameter, source-collection fiber separation distance, and fiber-tissue spacer thickness—on light propagation and the origin of detected fluorescence. An excitation wavelength of 400 nm and an emission wavelength of 630 nm were simulated. Noteworthy effects included an increase in axial selectivity with decreasing fiber size and a transition with increasing fiber-tissue spacer size from a subsurface peak in fluorophore sensitivity to a nearly monotonic decrease typical of single-fiber probes. We provide theoretical evidence that probe design strongly affects tissue interrogation. Therefore application-specific customization of probe design may lead to improvements in the efficacy of fluorescence-based diagnostic devices.
机译:光纤探头是许多定量荧光光谱系统的重要组成部分,可以在各种临床和实验室情况下提供激发光并收集反射的荧光。但是,关于照明收集几何形状如何指导这些组件的设计的信息很少。因此,我们使用蒙特卡洛模型研究了多纤维探针设计参数(数值孔径,纤维直径,源收集纤维分离距离和纤维组织间隔物厚度)对光传播和检测到的荧光源的影响。模拟了400 nm的激发波长和630 nm的发射波长。值得注意的影响包括轴向选择性随着纤维尺寸的减小而增加,以及随着纤维组织间隔尺寸的增加从荧光团敏感性的亚峰到单纤维探针的近乎单调减小的过渡。我们提供理论上的证据,探针设计强烈影响组织审讯。因此,探针设计的特定于应用的定制可以导致基于荧光的诊断装置的功效的提高。

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