胶质瘤
间充质干细胞
表型
恶性肿瘤
生物
癌症研究
体内
转录组
病理
细胞生物学
基因
基因表达
医学
生物化学
生物技术
作者
Andrea Comba,Syed M. Faisal,Patrick F. Dunn,Anna E Argento,Todd C. Hollon,Wajd N. Al-Holou,Maria Varela,Daniel Zamler,Gunnar Lennart Quass,Pierre F Apostolides,Christine E. Brown,Phillip E. Kish,Alon Kahana,Celina G. Kleer,Sebastien Motsch,Maria G. Castro,Pedro R. Lowenstein
标识
DOI:10.1101/2020.12.01.404970
摘要
ABSTRACT Intra-tumoral heterogeneity and diffuse infiltration are hallmarks of glioblastoma that challenge treatment efficacy. However, the mechanisms that set up both tumor heterogeneity and invasion remain poorly understood. Herein, we present a comprehensive spatiotemporal study that aligns distinctive intra-tumoral histopathological structures, oncostreams, with dynamic properties and a unique, actionable, spatial transcriptomic signature. Oncostreams are dynamic multicellular fascicles of spindle-like and aligned cells with mesenchymal properties, detected using ex vivo explants and in vivo intravital imaging. Their density correlates with tumor aggressiveness in genetically engineered mouse glioma models, and high-grade human gliomas. Oncostreams facilitate the intra-tumoral distribution of tumoral and non-tumoral cells, and the invasion of the normal brain. These fascicles are defined by a specific molecular signature that regulates their organization and function. Oncostreams structure and function depend on overexpression of COL1A1. COL1A1 is a central gene in the dynamic organization of glioma mesenchymal transformation, and a powerful regulator of glioma malignant behavior. Inhibition of COL1A1 eliminated oncostreams, reprogramed the malignant histopathological phenotype, reduced expression of the mesenchymal associated genes, induced changes in the tumor microenvironment and prolonged animal survival. Oncostreams represent a novel pathological marker of potential value for diagnosis, prognosis, and treatment.
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