Single Cell Data Enables Dissecting Cell Types Present in Bulk Transcriptome Data.

Stem cells and development Pub Date : 2025-01-01 Epub Date: 2024-11-29 DOI:10.1089/scd.2024.0152
Wasco Wruck, James Adjaye
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Abstract

The quality of organoid models can be assessed by single-cell-RNA-sequencing (scRNA-seq) but often only bulk transcriptome data is available. Here we present a pipeline for the analysis of scRNA-seq data and subsequent "deconvolution," which is a method for estimating cell type fractions in bulk transcriptome data based on expression profiles and cell types found in scRNA-seq data derived from biopsies. We applied this pipeline on bulk iPSC-derived kidney and brain organoid transcriptome data to identify cell types employing two scRNA-seq kidney datasets and one brain dataset. Relevant cells present in kidney (e.g., proximal tubules, distal convoluted tubules, and podocytes) and brain (e.g., neurons, astrocytes, oligodendrocytes, and microglia) with obligatory endothelial and immune-related cells were identified. We anticipate that this pipeline will also enable estimation of cell type fractions in organoids of other tissues.

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单细胞数据使解剖细胞类型存在于大量转录组数据。
类器官模型的质量可以通过单细胞rna测序(scRNA-seq)来评估,但通常只有大量转录组数据可用。在这里,我们提出了一个用于分析scRNA-seq数据和随后的“反卷积”的管道,这是一种基于来自活检的scRNA-seq数据中发现的表达谱和细胞类型来估计大量转录组数据中细胞类型部分的方法。我们使用两个scRNA-seq肾脏数据集和一个大脑数据集,将该管道应用于大量ipsc衍生的肾脏和脑类器官转录组数据,以鉴定细胞类型。相关细胞存在于肾脏(例如,近端小管,远端曲小管和足细胞)和大脑(例如,神经元,星形胶质细胞,少突胶质细胞和小胶质细胞)中,具有强制性内皮细胞和免疫相关细胞。我们预计,这一管道也将使其他组织的类器官的细胞类型分数的估计。
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