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应用二次谐波产生成像显微镜研究卵巢癌细胞外基质的改变。

Alterations of the extracellular matrix in ovarian cancer studied by Second Harmonic Generation imaging microscopy.

机构信息

Center for Cell Analysis and Modeling, Department of Cell Biology, University of Connecticut Health Center, Farmington, CT 06030, USA.

出版信息

BMC Cancer. 2010 Mar 11;10:94. doi: 10.1186/1471-2407-10-94.

Abstract

BACKGROUND

Remodeling of the extracellular matrix (ECM) has been implicated in ovarian cancer, and we hypothesize that these alterations may provide a better optical marker of early disease than currently available imaging/screening methods and that understanding their physical manifestations will provide insight into invasion.

METHODS

For this investigation we use Second Harmonic Generation (SHG) imaging microcopy to study changes in the structure of the ovarian ECM in human normal and malignant ex vivo biopsies. This method directly visualizes the type I collagen in the ECM and provides quantitative metrics of the fibrillar assembly. To quantify these changes in collagen morphology we utilized an integrated approach combining 3D SHG imaging measurements and bulk optical parameter measurements in conjunction with Monte Carlo simulations of the experimental data to extract tissue structural properties.

RESULTS

We find the SHG emission attributes (directionality and relative intensity) and bulk optical parameters, both of which are related to the tissue structure, are significantly different in the tumors in a manner that is consistent with the change in collagen assembly. The normal and malignant tissues have highly different collagen fiber assemblies, where collectively, our findings show that the malignant ovaries are characterized by lower cell density, denser collagen, as well as higher regularity at both the fibril and fiber levels. This further suggests that the assembly in cancer may be comprised of newly synthesized collagen as opposed to modification of existing collagen.

CONCLUSIONS

Due to the large structural changes in tissue assembly and the SHG sensitivity to these collagen alterations, quantitative discrimination is achieved using small patient data sets. Ultimately these measurements may be developed as intrinsic biomarkers for use in clinical applications.

摘要

背景

细胞外基质(ECM)的重塑与卵巢癌有关,我们假设这些改变可能比目前可用的成像/筛查方法提供更好的早期疾病光学标志物,并且了解它们的物理表现将为侵袭提供深入了解。

方法

为了进行这项研究,我们使用二次谐波产生(SHG)成像显微镜来研究人类正常和恶性离体活检中卵巢 ECM 结构的变化。该方法直接可视化 ECM 中的 I 型胶原,并提供纤维组装的定量指标。为了量化胶原形态的这些变化,我们利用了一种结合 3D SHG 成像测量和体光学参数测量的综合方法,并结合实验数据的蒙特卡罗模拟来提取组织结构特性。

结果

我们发现 SHG 发射属性(方向性和相对强度)和体光学参数,这两者都与组织结构相关,在肿瘤中以与胶原组装变化一致的方式显著不同。正常和恶性组织具有高度不同的胶原纤维组装,我们的研究结果表明,恶性卵巢的特征是细胞密度降低、胶原密度增加以及纤维和纤维水平的规则性更高。这进一步表明,癌症中的组装可能由新合成的胶原蛋白组成,而不是现有胶原蛋白的修饰。

结论

由于组织组装的结构发生了巨大变化,并且 SHG 对这些胶原改变具有敏感性,因此可以使用小的患者数据集进行定量区分。最终,这些测量值可能会被开发为用于临床应用的内在生物标志物。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/a524/2841668/d6bcf46f3072/1471-2407-10-94-1.jpg

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