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开发一种用于分析人韧带中感觉神经末梢的 3D 免疫荧光分析方法。

Development of a 3D-immunofluorescence analysis for sensory nerve endings in human ligaments.

机构信息

Department of Plastic and Hand Surgery, Burn Unit, Klinikum Sankt Georg, Delitzscher Straße 141, 04129 Leipzig, Germany; Martin-Luther-University Halle-Wittenberg, Germany.

Martin-Luther-University Halle-Wittenberg, Germany; Department of Plastic and Hand Surgery with Burn Unit, Trauma Center Bergmannstrost, 06112 Halle, Germany.

出版信息

J Neurosci Methods. 2022 Dec 1;382:109724. doi: 10.1016/j.jneumeth.2022.109724. Epub 2022 Oct 4.

Abstract

BACKGROUND

The analysis of ligamentous mechanoreceptors is difficult due to a high amount of unclassifiable mechanoreceptors, which result from incomplete visualization through limited microscopic techniques.

NEW METHOD

The method was developed using dorsal intercarpal ligaments and dorsal regions of the scapholunate interosseous ligament from human cadaver wrists. Consecutive 70 µm thick cryosections were stained with immunofluorescence markers for protein S100B, neurotrophin receptor p75 (p75), protein gene product 9.5 (PGP 9.5) and 4',6-diamidino-2-phenylindole (DAPI). 3D images of sensory nerve endings were obtained using a confocal laser scanning microscope. Experimental point spread functions (PSF) were used to deconvolve images. Sensory nerve endings were localised in each section plane and classified according to Freeman and Wyke. Finally, confocal data was visualized as 3D-images.

RESULTS

The method produced excellent image quality, revealing detailed three-dimensional structures. The created 3D-model of sensory nerve endings could be analyzed in all three dimensions, augmenting visualization of the form and immunoreactive pattern of sensory nerve endings. Deconvolution with experimentally measured PSFs aided in enhancing image quality.

COMPARISON WITH EXISTING METHODS

Using a triple immunofluorescent staining method allows to visualize the structure of sensory nerve endings more precisely than techniques with serial analysis of different monostaining of neural markers. Imaging in three dimensions enhances morphologic details, which are limited in 2D-microscopy.

CONCLUSION

3D-triple immunofluorescence produces high quality visualization of mechanoreceptors, thereby improving their analysis. As an elaborate technique, it is ideal for defined research questions concerning the microstructure of sensory nerve endings.

摘要

背景

由于通过有限的显微镜技术无法完全可视化,导致大量未分类的机械感受器,因此分析韧带机械感受器具有一定难度。

新方法

该方法是使用人尸体手腕的背侧腕间韧带和舟月骨间背侧韧带开发的。连续的 70µm 厚的冷冻切片用免疫荧光标记物进行染色,用于 S100B 蛋白、神经营养素受体 p75(p75)、蛋白基因产物 9.5(PGP 9.5)和 4',6-二脒基-2-苯基吲哚(DAPI)。使用共聚焦激光扫描显微镜获取感觉神经末梢的 3D 图像。使用实验点扩散函数(PSF)对图像进行反卷积。在每个截面平面中定位感觉神经末梢,并根据 Freeman 和 Wyke 进行分类。最后,将共聚焦数据可视化作为 3D 图像。

结果

该方法产生了出色的图像质量,显示了详细的三维结构。创建的感觉神经末梢 3D 模型可以在所有三个维度上进行分析,增强了对感觉神经末梢形态和免疫反应模式的可视化。使用实验测量的 PSF 进行反卷积有助于提高图像质量。

与现有方法的比较

使用三重免疫荧光染色方法可以比使用连续分析不同神经标记物的单染色技术更精确地显示感觉神经末梢的结构。三维成像增强了形态细节,而二维显微镜则受到限制。

结论

3D 三重免疫荧光可产生高质量的机械感受器可视化效果,从而改善其分析。作为一种精细的技术,它非常适合有关感觉神经末梢微观结构的明确研究问题。

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