复发性高级别胶质瘤非增强区的单核表达特征。

IF 3.7 Q1 CLINICAL NEUROLOGY
Neuro-oncology advances Pub Date : 2024-01-25 eCollection Date: 2024-01-01 DOI:10.1093/noajnl/vdae005
Kunal S Patel, Kaleab K Tessema, Riki Kawaguchi, Lindsey Dudley, Alvaro G Alvarado, Sree Deepthi Muthukrishnan, Travis Perryman, Akifumi Hagiwara, Vivek Swarup, Linda M Liau, Anthony C Wang, William Yong, Daniel H Geschwind, Ichiro Nakano, Steven A Goldman, Richard G Everson, Benjamin M Ellingson, Harley I Kornblum
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引用次数: 0

摘要

背景:方法:我们利用单核 RNA 测序技术对 15 例复发性高级别胶质瘤标本(n = 5)进行了比较:我们利用单核 RNA 测序技术对 15 份复发高级别胶质瘤标本(n = 5)进行了分析,比较了从 CE 和 NE 区域获得的前瞻性活检标本。此外,还对 24 例 CE 和 22 例 NE 活检样本进行了免疫组化染色,以验证 RNA 结果:结果:NE区域的肿瘤细胞富含神经祖细胞样细胞状态,而CE区域的肿瘤细胞富含间充质样细胞状态。相对于CE区域,NE胶质瘤细胞中增殖细胞和推定胶质瘤干细胞的比例相似,但Ki-67染色%无显著差异。NE区域的肿瘤细胞表现出以前与低级别胶质瘤相关的基因上调。我们在复发性GBM中的发现与对原发性GBM数据集的重新分析中的一些发现相似。对东北区域肿瘤微环境的细胞、基因和通路水平分析显示,肿瘤介导的新生血管和细胞介导的免疫反应相对下调,但胶质瘤与非病理细胞的相互作用增加:这项综合分析说明了高级别胶质瘤中CE区和NE区不同的肿瘤和非肿瘤景观,强调了NE区是一个可能在促肿瘤微环境中引发复发的区域,并为未来设计NE特异性辅助疗法确定了可能的靶点。这些研究结果还支持采用积极的方法切除带有肿瘤的东北部区域。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
Single-nucleus expression characterization of non-enhancing region of recurrent high-grade glioma.

Background: Non-enhancing (NE) infiltrating tumor cells beyond the contrast-enhancing (CE) bulk of tumor are potential propagators of recurrence after gross total resection of high-grade glioma.

Methods: We leveraged single-nucleus RNA sequencing on 15 specimens from recurrent high-grade gliomas (n = 5) to compare prospectively identified biopsy specimens acquired from CE and NE regions. Additionally, 24 CE and 22 NE biopsies had immunohistochemical staining to validate RNA findings.

Results: Tumor cells in NE regions are enriched in neural progenitor cell-like cellular states, while CE regions are enriched in mesenchymal-like states. NE glioma cells have similar proportions of proliferative and putative glioma stem cells relative to CE regions, without significant differences in % Ki-67 staining. Tumor cells in NE regions exhibit upregulation of genes previously associated with lower grade gliomas. Our findings in recurrent GBM paralleled some of the findings in a re-analysis of a dataset from primary GBM. Cell-, gene-, and pathway-level analyses of the tumor microenvironment in the NE region reveal relative downregulation of tumor-mediated neovascularization and cell-mediated immune response, but increased glioma-to-nonpathological cell interactions.

Conclusions: This comprehensive analysis illustrates differing tumor and nontumor landscapes of CE and NE regions in high-grade gliomas, highlighting the NE region as an area harboring likely initiators of recurrence in a pro-tumor microenvironment and identifying possible targets for future design of NE-specific adjuvant therapy. These findings also support the aggressive approach to resection of tumor-bearing NE regions.

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CiteScore
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