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单细胞转录组揭示人类癌症中细胞类型特异性和样本特异性基因功能。

Single-cell transcriptomes reveal cell-type-specific and sample-specific gene function in human cancer.

作者信息

Yuan Huating, Liang Xin, Zhang Xinxin, Cao Yu

机构信息

College of Biology and Engineering, Guizhou Medical University, Guiyang, China.

College of Bioinformatics Science and Technology, Harbin Medical University, Harbin, China.

出版信息

Heliyon. 2025 Jan 23;11(3):e42218. doi: 10.1016/j.heliyon.2025.e42218. eCollection 2025 Feb 15.

Abstract

Accurate annotation of gene function in individual samples and even in each cell type is essential for understanding the pathogenesis of cancers. Single-cell RNA-sequencing (scRNA-seq) provides unprecedented resolution to decipher gene function. In order to explore how scRNA-seq contributes to the understanding of gene function in cancers, we constructed an assessment framework based on co-expression network and neighbor-voting method using 116,814 cells. Compared with bulk transcriptome, scRNA-seq recalled more experimentally verified gene functions. Surprisingly, scRNA-seq revealed cell-type-specific functions, especially in immune cells, whose expression profile recalled immune-related functions that were not discovered in cancer cells. Furthermore, scRNA-seq discovered sample-specific functions, highlighting that it provided sample-specific information. We also explored factors affecting the performance of gene function prediction. We found that 500 or more cells should be considered in the prediction with scRNA-seq, and that scRNA-seq datasets generated from 10x Genomics platform had a better performance than those from Smart-seq2. Collectively, we compared the prediction performance of bulk data and scRNA-seq data from multiple perspectives, revealing the irreplaceable role of single-cell sequencing in decoding the biological progresses in which the gene involved.

摘要

准确注释个体样本甚至每种细胞类型中的基因功能对于理解癌症的发病机制至关重要。单细胞RNA测序(scRNA-seq)为破译基因功能提供了前所未有的分辨率。为了探索scRNA-seq如何有助于理解癌症中的基因功能,我们使用116,814个细胞构建了一个基于共表达网络和邻居投票方法的评估框架。与批量转录组相比,scRNA-seq召回了更多经过实验验证的基因功能。令人惊讶的是,scRNA-seq揭示了细胞类型特异性功能,尤其是在免疫细胞中,其表达谱召回了在癌细胞中未发现的免疫相关功能。此外,scRNA-seq发现了样本特异性功能,突出表明它提供了样本特异性信息。我们还探讨了影响基因功能预测性能的因素。我们发现,在使用scRNA-seq进行预测时应考虑500个或更多细胞,并且从10x Genomics平台生成的scRNA-seq数据集比来自Smart-seq2的数据集具有更好的性能。总体而言,我们从多个角度比较了批量数据和scRNA-seq数据的预测性能,揭示了单细胞测序在解码基因参与的生物学进程中的不可替代作用。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/03eb/11830296/f359ba85b64c/ga1.jpg

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