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偏振分辨非线性显微镜中光散射的定量分析。

Quantitative analysis of light scattering in polarization-resolved nonlinear microscopy.

作者信息

de Aguiar Hilton B, Gasecka Paulina, Brasselet Sophie

出版信息

Opt Express. 2015 Apr 6;23(7):8960-73. doi: 10.1364/OE.23.008960.

Abstract

Polarization resolved nonlinear microscopy (PRNM) is a powerful technique to gain microscopic structural information in biological media. However, deep imaging in a variety of biological specimens is hindered by light scattering phenomena, which not only degrades the image quality but also affects the polarization state purity. In order to quantify this phenomenon and give a framework for polarization resolved microscopy in thick scattering tissues, we develop a characterization methodology based on four wave mixing (FWM) process. More specifically, we take advantage of two unique features of FWM, meaning its ability to produce an intrinsic in-depth local coherent source and its capacity to quantify the presence of light depolarization in isotropic regions inside a sample. By exploring diverse experimental layouts in phantoms with different scattering properties, we study systematically the influence of scattering on the nonlinear excitation and emission processes. The results show that depolarization mechanisms for the nonlinearly generated photons are highly dependent on the scattering center size, the geometry used (epi/forward) and, most importantly, on the thickness of the sample. We show that the use of an un-analyzed detection makes the polarization-dependence read-out highly robust to scattering effects, even in regimes where imaging might be degraded. The effects are illustrated in polarization resolved imaging of myelin lipid organization in mouse spinal cords.

摘要

偏振分辨非线性显微镜(PRNM)是一种在生物介质中获取微观结构信息的强大技术。然而,各种生物样本中的深度成像受到光散射现象的阻碍,这不仅会降低图像质量,还会影响偏振态纯度。为了量化这种现象并为厚散射组织中的偏振分辨显微镜提供一个框架,我们开发了一种基于四波混频(FWM)过程的表征方法。更具体地说,我们利用了FWM的两个独特特性,即其产生内在深度局部相干源的能力以及量化样品内部各向同性区域中光去极化存在的能力。通过在具有不同散射特性的模型中探索不同的实验布局,我们系统地研究了散射对非线性激发和发射过程的影响。结果表明,非线性产生光子的去极化机制高度依赖于散射中心尺寸、所使用的几何结构(反射/前向),最重要的是,依赖于样品的厚度。我们表明,即使在成像可能退化的情况下,使用未经分析的检测也能使偏振依赖性读出对散射效应具有高度鲁棒性。这些效应在小鼠脊髓髓磷脂脂质组织的偏振分辨成像中得到了说明。

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