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基于单细胞成像的肿瘤进展染色质生物标志物。

Single cell imaging-based chromatin biomarkers for tumor progression.

机构信息

Mechanobiology Institute and Department of Biological Sciences, National University of Singapore, Singapore, 117411, Singapore.

Department of Health Sciences and Technology, ETH Zurich, Zurich, Switzerland.

出版信息

Sci Rep. 2021 Nov 29;11(1):23041. doi: 10.1038/s41598-021-02441-6.

Abstract

Tumour progression within the tissue microenvironment is accompanied by complex biomechanical alterations of the extracellular environment. While histopathology images provide robust biochemical markers for tumor progression in clinical settings, a quantitative single cell score using nuclear morphology and chromatin organization integrated with the long range mechanical coupling within the tumor microenvironment is missing. We propose that the spatial chromatin organization in individual nuclei characterises the cell state and their alterations during tumor progression. In this paper, we first built an image analysis pipeline and implemented it to classify nuclei from patient derived breast tissue biopsies of various cancer stages based on their nuclear and chromatin features. Replacing H&E with DNA binding dyes such as Hoescht stained tissue biopsies, we improved the classification accuracy. Using the nuclear morphology and chromatin organization features, we constructed a pseudo-time model to identify the chromatin state changes that occur during tumour progression. This enabled us to build a single-cell mechano-genomic score that characterises the cell state during tumor progression from a normal to a metastatic state. To gain further insights into the alterations in the local tissue microenvironments, we also used the nuclear orientations to identify spatial neighbourhoods that have been posited to drive tumor progression. Collectively, we demonstrate that image-based single cell chromatin and nuclear features are important single cell biomarkers for phenotypic mapping of tumor progression.

摘要

肿瘤在组织微环境中的进展伴随着细胞外环境的复杂生物力学改变。虽然组织病理学图像为临床环境中的肿瘤进展提供了强大的生化标志物,但缺乏使用核形态和染色质组织与肿瘤微环境中的长程力学耦合并整合的定量单细胞评分。我们提出,单个核中的空间染色质组织特征化了细胞状态及其在肿瘤进展过程中的变化。在本文中,我们首先构建了一个图像分析管道,并将其实现为根据核和染色质特征对来自不同癌症阶段的患者衍生的乳腺组织活检中的核进行分类。通过用 DNA 结合染料(如 Hoechst 染色组织活检)代替 H&E,我们提高了分类准确性。使用核形态和染色质组织特征,我们构建了一个伪时间模型来识别肿瘤进展过程中发生的染色质状态变化。这使我们能够构建一个单细胞机械基因组评分,该评分描述了从正常到转移状态的肿瘤进展过程中的细胞状态。为了更深入地了解局部组织微环境的改变,我们还使用核取向来识别被认为推动肿瘤进展的空间邻域。总之,我们证明了基于图像的单细胞染色质和核特征是肿瘤进展表型图谱的重要单细胞生物标志物。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/36bb/8630115/fea70af1f10f/41598_2021_2441_Fig1_HTML.jpg

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