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首页> 外文期刊>Journal of Applied Physics >Fully automated, quantitative, noninvasive assessment of collagen fiber content and organization in thick collagen gels
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Fully automated, quantitative, noninvasive assessment of collagen fiber content and organization in thick collagen gels

机译:全自动,定量,无创性评估厚胶原蛋白凝胶中胶原纤维的含量和组织

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摘要

Collagen is the most prominent protein of human tissues. Its content and organization define to a large extent the mechanical properties of tissue as well as its function. Methods that have been used traditionally to visualize and analyze collagen are invasive, provide only qualitative or indirect information, and have limited use in studies that aim to understand the dynamic nature of collagen remodeling and its interactions with the surrounding cells and other matrix components. Second harmonic generation (SHG) imaging emerged as a promising noninvasive modality for providing high-resolution images of collagen fibers within thick specimens, such as tissues. In this article, we present a fully automated procedure to acquire quantitative information on the content, orientation, and organization of collagen fibers. We use this procedure to monitor the dynamic remodeling of collagen gels in the absence or presence of fibroblasts over periods of 12 or 14 days. We find that an adaptive thresholding and stretching approach provides great insight to the content of collagen fibers within SHG images without the need for user input. An additional feature-erosion and feature-dilation step is useful for preserving structure and noise removal in images with low signal. To quantitatively assess the orientation of collagen fibers, we extract the orientation index (OI), a parameter based on the power distribution of the spatial-frequency-averaged, two-dimensional Fourier transform of the SHG images. To measure the local organization of the collagen fibers, we access the Hough transform of small tiles of the image and compute the entropy distribution, which represents the probability of finding the direction of fibers along a dominant direction. Using these methods we observed that the presence and number of fibroblasts within the collagen gel significantly affects the remodeling of the collagen matrix. In the absence of fibroblasts, gels contract, especially during the first few days, in a manner that allows the fibers to remain mostly disoriented, as indicated by small OI values. Subtle changes in the local organization of fibers may be taking place as the corresponding entropy values of these gels show a small decrease. The presence of fibroblasts affects the collagen matrix in a manner that is highly dependent on their number. A low density of fibroblasts enhances the rate of initial gel contraction, but ultimately leads to degradation of collagen fibers, which start to organize in localized clumps. This degradation and reorganization is seen within the first days of incubation with fibroblasts at a high density and is followed by de novo collagen fiber deposition by the fibroblasts. These collagen fibers are more highly oriented and organized than the fibers of the original collagen gel. These initial studies demonstrate that SHG imaging in combination with automated image analysis approaches offer a noninvasive and easily implementable method for characterizing important features of the content and organization of collagen in tissuelike specimens. Therefore, these studies could offer important insights for improving tissue engineering and disease diagnostic efforts.
机译:胶原蛋白是人体组织中最突出的蛋白质。它的含量和组织在很大程度上定义了组织的机械特性及其功能。传统上用于可视化和分析胶原蛋白的方法具有侵入性,仅提供定性或间接信息,并且在旨在了解胶原蛋白重构的动态特性及其与周围细胞和其他基质成分相互作用的研究中用途有限。二次谐波生成(SHG)成像已成为一种有前途的无创模式,可用于在厚样本(例如组织)中提供胶原纤维的高分辨率图像。在本文中,我们提出了一个全自动程序,以获取有关胶原纤维的含量,方向和组织的定量信息。我们使用此程序来监视在不存在或存在成纤维细胞的情况下,在12或14天的时间内胶原蛋白凝胶的动态重塑。我们发现,自适应阈值化和拉伸方法无需用户输入即可深入了解SHG图像中胶原纤维的含量。附加的特征侵蚀和特征扩张步骤对于保留低信号图像中的结构和噪声去除很有用。为了定量评估胶原纤维的取向,我们提取取向指数(OI),该参数基于SHG图像的空间频率平均二维傅立叶变换的功率分布。为了测量胶原纤维的局部组织,我们访问图像的小图块的霍夫变换并计算熵分布,这表示找到沿主要方向的纤维方向的可能性。使用这些方法,我们观察到胶原蛋白凝胶中成纤维细胞的存在和数量显着影响胶原蛋白基质的重塑。在不存在成纤维细胞的情况下,凝胶收缩,尤其是在最初的几天内,以某种方式收缩,使纤维保持大部分方向保持不定向,如OI值小所示。纤维的局部组织可能发生细微变化,因为这些凝胶的相应熵值显示出较小的下降。成纤维细胞的存在以高度依赖于其数目的方式影响胶原基质。低密度的成纤维细胞增加了初始凝胶收缩的速率,但最终导致胶原纤维降解,胶原纤维开始在局部团块中组织。在以高密度与成纤维细胞一起孵育的第一天就可以看到这种降解和重组,随后成纤维细胞从头开始沉积胶原纤维。这些胶原纤维比原始胶原凝胶的纤维具有更高的取向性和组织性。这些初步研究表明,SHG成像结合自动图像分析方法可提供一种无创且易于实施的方法,用于表征组织样标本中胶原含量和组织的重要特征。因此,这些研究可为改善组织工程和疾病诊断工作提供重要的见识。

著录项

  • 来源
    《Journal of Applied Physics》 |2009年第10期|102042.1-102042.11|共11页
  • 作者单位

    Department of Biomedical Engineering, Tufts University, Medford, Massachusetts 02155, USA;

    Department of Biomedical Engineering, Tufts University, Medford, Massachusetts 02155, USA;

    Department of Electrical and Computer Engineering, Tufts University, Medford, Masachusetts 02155, USA;

    Department of Biomedical Engineering, Tufts University, Medford, Massachusetts 02155, USA;

    Department of Biomedical Engineering, Tufts University, Medford, Massachusetts 02155, USA;

  • 收录信息 美国《科学引文索引》(SCI);美国《工程索引》(EI);美国《生物学医学文摘》(MEDLINE);
  • 原文格式 PDF
  • 正文语种 eng
  • 中图分类
  • 关键词

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