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Multiscale analysis of polarization-resolved third-harmonic generation microscopy from ordered lipid assemblies

机译:从有序脂质组装物中偏振分辨的三次谐波产生显微镜的多尺度分析

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Nonlinear optical microscopy is a biocompatible avenue for probing ordered molecular assemblies in biological tissues. As in linear optics, the nonlinear optical response from ordered systems is polarization-sensitive. This dependence can be used to identify and characterize local molecular ordering with micrometer-scale 3D resolution in a nonlinear microscope. In particular, third-harmonic generation (THG) microscopy is a nonlinear optical modality sensitive to the electronic nonlinear susceptibility x~((3)) of a material. THG microscopy can be used to map x~((3)) spatial variations (i.e. material interfaces), and to probe birefringence. In principle, polarization-resolved THG (P-THG) can therefore be used to probe ordered molecular arrays. However, the orientation, distribution, and nonlinear optical properties of the molecules near the beam focus all affect the detected signal. It is therefore necessary to develop a theoretical method which decouples these effects and permits the extraction of orientational information from P-THG images. In this report, we first present P-THG images of model systems (lipid droplets, multilamellar lipid vesicles) and biological tissues (human skin biopsy) which establish that P-THG is sensitive to lipid ordering and that it is maximized when excitation polarization is parallel to the ordered lipid molecules, giving impetus for the development of a thorough theoretical analysis. We then outline a multiscale model spanning the molecular (nm) and ensemble (μm) scales predicting the P-THG signal, consisting of three main steps: (ⅰ) calculation of the molecular electronic hyperpolarizability; (ⅱ) determination of the anisotropic x~((3)) for various molecular distribution parameters; and (ⅲ) numerical calculations of the P-THG signal from lipid-water interfaces. This analysis links the measured P-THG response to lipid molecular structure and ordering.
机译:非线性光学显微镜是一种用于探测生物组织中有序分子组装的生物相容性途径。与线性光学一样,有序系统的非线性光学响应对偏振敏感。这种依赖性可用于在非线性显微镜中以微米级3D分辨率识别和表征局部分子有序。特别地,三次谐波产生(THG)显微镜是对材料的电子非线性磁化率x〜((3))敏感的非线性光学模态。 THG显微镜可用于绘制x〜((3))空间变化(即材料界面)并探测双折射。原则上,偏振分辨THG(P-THG)因此可用于探测有序分子阵列。但是,光束焦点附近分子的方向,分布和非线性光学特性都会影响检测到的信号。因此,有必要开发一种理论方法,该方法将这些效应解耦并允许从P-THG图像中提取方向信息。在本报告中,我们首先介绍模型系统(脂质液滴,多层脂质囊泡)和生物组织(人体皮肤活检)的P-THG图像,这些图像确定P-THG对脂质有序敏感,并且在激发极化作用下最大。平行于有序的脂质分子,为彻底的理论分析的发展提供了动力。然后,我们概述了一个跨越分子(nm)和集合(μm)尺度的多尺度模型,该模型可预测P-THG信号,包括三个主要步骤:(ⅰ)计算分子电子的超极化性; (ⅱ)确定各种分子分布参数的各向异性x〜((3)); (ⅲ)来自脂质-水界面的P-THG信号的数值计算。该分析将测得的P-THG反应与脂质分子结构和有序联系起来。

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