Integrated bulk and single-cell RNA-sequencing identified disease-relevant monocytes and a gene network module underlying systemic sclerosis

免疫系统 基因 转录组 单细胞分析 基因表达 细胞 免疫学 流式细胞术 计算生物学 核糖核酸 生物 遗传学
作者
Satomi Kobayashi,Yasuo Nagafuchi,Masaaki Okubo,Yusuke Sugimori,Hiroko Shirai,Hiroaki Hatano,Joji Maeda,Haruyuki Yanaoka,Yusuke Takeshima,Ota M,Yoichi Iwasaki,Shuji Sumitomo,Tomohisa Okamura,Kazuhiko Yamamoto,Hirofumi Shoda,Keishi Fujio
出处
期刊:Journal of Autoimmunity [Elsevier]
卷期号:116: 102547-102547 被引量:25
标识
DOI:10.1016/j.jaut.2020.102547
摘要

Immunological disturbances have been reported in systemic sclerosis (SSc). This study assessed the transcriptome disturbances in immune cell subsets in SSc and characterized a disease-related gene network module and immune cell cluster at single cell resolution. Twenty-one Japanese SSc patients were enrolled and compared with 13 age- and sex-matched healthy controls (HC). Nineteen peripheral blood immune cell subsets were sorted by flow cytometry and bulk RNA-seq analysis was performed for each. Differential expression and pathway analyses were conducted. Iterative weighted gene correlation network analysis (iWGCNA) of each subset revealed clustered co-expressed gene network modules. Random forest analysis prioritized a disease-related gene module. Single cell RNA-seq analysis of 878 monocytes was integrated with bulk RNA-seq analysis and with a public database for single cell RNA-seq analysis of SSc patients. Inflammatory pathway genes were differentially expressed in widespread immune cell subsets of SSc. An inflammatory gene module from CD16+ monocytes, which included KLF10, PLAUR, JUNB and JUND, showed the greatest discrimination between SSc and HC. One of the clusters of SSc monocytes identified by single-cell RNA-seq analysis characteristically expressed these inflammatory co-expressed genes and was similar to lung infiltrating FCN1hi monocytes expressing IL1B. Our integrated analysis of bulk and single cell RNA-seq analysis identified an inflammatory gene module and a cluster of monocytes that are relevant to SSc pathophysiology. They could serve as candidate novel therapeutic targets in SSc.
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