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Metabolic landscape of the tumor microenvironment at single cell resolution

机译:单细胞分辨率下肿瘤微环境的代谢态势

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摘要

The tumor milieu consists of numerous cell types each existing in a different environment. However, a characterization of metabolic heterogeneity at single-cell resolution is not established. Here, we develop a computational pipeline to study metabolic programs in single cells. In two representative human cancers, melanoma and head and neck, we apply this algorithm to define the intratumor metabolic landscape. We report an overall discordance between analyses of single cells and those of bulk tumors with higher metabolic activity in malignant cells than previously appreciated. Variation in mitochondrial programs is found to be the major contributor to metabolic heterogeneity. Surprisingly, the expression of both glycolytic and mitochondrial programs strongly correlates with hypoxia in all cell types. Immune and stromal cells could also be distinguished by their metabolic features. Taken together this analysis establishes a computational framework for characterizing metabolism using single cell expression data and defines principles of the tumor microenvironment.
机译:肿瘤环境由多种细胞类型组成,每种细胞类型都存在于不同的环境中。但是,尚未建立在单细胞分辨率下代谢异质性的表征。在这里,我们开发了一条计算管线来研究单细胞中的代谢程序。在两种代表性的人类癌症中,黑色素瘤和头部和颈部,我们应用此算法来定义肿瘤内代谢情况。我们报告单细胞分析与恶性细胞中代谢活性高于先前认识的大块肿瘤分析之间的总体矛盾。线粒体程序的变化被发现是代谢异质性的主要贡献者。令人惊讶的是,糖酵解和线粒体程序的表达在所有细胞类型中均与缺氧密切相关。免疫细胞和基质细胞也可以通过它们的代谢特征来区分。综上所述,该分析建立了使用单细胞表达数据表征代谢的计算框架,并定义了肿瘤微环境的原理。

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