通过对高级别浆液性卵巢肿瘤标本进行多区域采样揭示的广泛三维肿瘤内蛋白质组异质性

Extensive three-dimensional intratumor proteomic heterogeneity revealed by multiregion sampling in high-grade serous ovarian tumor specimens.

作者信息

Hunt Allison L, Bateman Nicholas W, Barakat Waleed, Makohon-Moore Sasha, Hood Brian L, Conrads Kelly A, Zhou Ming, Calvert Valerie, Pierobon Mariaelena, Loffredo Jeremy, Litzi Tracy J, Oliver Julie, Mitchell Dave, Gist Glenn, Rojas Christine, Blanton Brian, Robinson Emma L, Odunsi Kunle, Sood Anil K, Casablanca Yovanni, Darcy Kathleen M, Shriver Craig D, Petricoin Emanuel F, Rao Uma N M, Maxwell G Larry, Conrads Thomas P

机构信息

Women's Health Integrated Research Center, Inova Women's Service Line, Inova Health System, 3289 Woodburn Road, Annandale, VA 22042, USA.

Gynecologic Cancer Center of Excellence, Department of Gynecologic Surgery and Obstetrics, Uniformed Services University and Walter Reed National Military Medical Center, 8901 Wisconsin Avenue, Bethesda, MD 20889, USA.

出版信息

iScience. 2021 Jun 21;24(7):102757. doi: 10.1016/j.isci.2021.102757. eCollection 2021 Jul 23.

DOI:10.1016/j.isci.2021.102757

PMID:34278265

原文链接:https://pmc.ncbi.nlm.nih.gov/articles/PMC8264160/

Abstract

Enriched tumor epithelium, tumor-associated stroma, and whole tissue were collected by laser microdissection from thin sections across spatially separated levels of ten high-grade serous ovarian carcinomas (HGSOCs) and analyzed by mass spectrometry, reverse phase protein arrays, and RNA sequencing. Unsupervised analyses of protein abundance data revealed independent clustering of an enriched stroma and enriched tumor epithelium, with whole tumor tissue clustering driven by overall tumor "purity." Comparing these data to previously defined prognostic HGSOC molecular subtypes revealed protein and transcript expression from tumor epithelium correlated with the differentiated subtype, whereas stromal proteins (and transcripts) correlated with the mesenchymal subtype. Protein and transcript abundance in the tumor epithelium and stroma exhibited decreased correlation in samples collected just hundreds of microns apart. These data reveal substantial tumor microenvironment protein heterogeneity that directly bears on prognostic signatures, biomarker discovery, and cancer pathophysiology and underscore the need to enrich cellular subpopulations for expression profiling.

摘要

通过激光显微切割从十个高级别浆液性卵巢癌（HGSOC）空间分离水平的薄切片中收集富集的肿瘤上皮、肿瘤相关基质和整个组织，并通过质谱、反相蛋白质阵列和RNA测序进行分析。对蛋白质丰度数据的无监督分析揭示了富集基质和富集肿瘤上皮的独立聚类，整个肿瘤组织的聚类由总体肿瘤“纯度”驱动。将这些数据与先前定义的预后HGSOC分子亚型进行比较，发现肿瘤上皮的蛋白质和转录物表达与分化亚型相关，而基质蛋白（和转录物）与间充质亚型相关。在仅相隔数百微米收集的样本中，肿瘤上皮和基质中的蛋白质和转录物丰度相关性降低。这些数据揭示了大量与预后特征、生物标志物发现和癌症病理生理学直接相关的肿瘤微环境蛋白质异质性，并强调了富集细胞亚群进行表达谱分析的必要性。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/2f37/8264160/2fe2a03e4e95/fx1.jpg

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通过对高级别浆液性卵巢肿瘤标本进行多区域采样揭示的广泛三维肿瘤内蛋白质组异质性

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