Residential College | false |
Status | 已發表Published |
Integrated Analysis of Single-Cell and Bulk RNA Sequencing Reveals Pro-Fibrotic PLA2G7(High) Macrophages in Pulmonary Fibrosis | |
Wang JunYi1,2,3; Jiang ManLing1,2; Xiong AnYing1,2; Zhang Lei1,2,3; LuoLi1; LiuYao1; Liu ShengBin1; Ran Qin1,2; Wu DeHong2; Xiong Ying4; He Xiang1,2; Leung Elaine Lai Han5; Li GuoPing1,2 | |
2022-08 | |
Source Publication | PHARMACOLOGICAL RESEARCH |
ISSN | 1043-6618 |
Volume | 182Pages:106286 |
Abstract | Pulmonary fibrosis (PF) is the pathological change of end-stage interstitial lung diseases with high mortality and limited therapeutic options. Lung macrophages have distinct subsets with divergent functions, and play critical roles in the pathogenesis of PF. In this study, integrative analysis of lung single-cell and bulk RNA-seq data from patients with fibrotic hypersensitivity pneumonitis and idiopathic pulmonary fibrosis was utilized to identify particular macrophage subsets during the development of PF. We find a specific macrophage subpopulation highly expressing PLA2G7 in fibrotic lungs. We performed additional single-cell RNA-seq analysis to identify analogous macrophage population in bleomycin (BLM)-induced mouse pulmonary fibrosis models. By in vitro and in vivo experiments, we further reveal the pro-fibrotic role for this PLA2G7(high) macrophage subset in fibroblastto-myofibroblast transition (FMT) during pulmonary fibrosis. PLA2G7 promotes FMT via LPC/ATX/LPA/LPA2 axis in macrophages. Moreover, PLA2G7 is regulated by STAT1, and pharmacological inhibition of PLA2G7 by Darapladib ameliorates pulmonary fibrosis in BLM-induced mice. The results of this study support the view that PLA2G7(high) macrophage subpopulation contributes importantly to the pathogenesis of PF, which provides a potential way for targeted therapy. |
Keyword | Pulmonary Fibrosis Fibroblast-to-myofibroblast Transition Macrophage Pla2g7 Single-cell Rna-seq |
DOI | 10.1016/j.phrs.2022.106286 |
URL | View the original |
Indexed By | SCIE |
WOS Research Area | Pharmacology & Pharmacy |
WOS Subject | Pharmacology & Pharmacy |
WOS ID | WOS:000810359600002 |
Scopus ID | 2-s2.0-85131366714 |
Fulltext Access | |
Citation statistics | |
Document Type | Journal article |
Collection | DEPARTMENT OF BIOMEDICAL SCIENCES INSTITUTE OF COLLABORATIVE INNOVATION |
Corresponding Author | He Xiang; Leung Elaine Lai Han; Li GuoPing |
Affiliation | 1.Laboratory of Allergy and Precision Medicine, Chengdu Institute of Respiratory Health, the Third People’s Hospital of Chengdu, Affiliated Hospital of Southwest Jiaotong University, Chengdu, China 2.Department of Pulmonary and Critical Care Medicine, Chengdu Institute of Respiratory Health, Chengdu Third People’s Hospital Branch of National Clinical Research Center for Respiratory Disease, Chengdu, China 3.State Key Laboratory of Quality Research in Chinese Medicine, Macau University of Science & Technology, Taipa, Macao Special Administrative Region of China 4.Department of Pulmonary and Critical Care Medicine, Sichuan Friendship Hospital, Chengdu, China 5.Faculty of Health Sciences, University of Macau, Taipa, Macao Special Administrative Region of China |
First Author Affilication | University of Macau |
Corresponding Author Affilication | Faculty of Health Sciences |
Recommended Citation GB/T 7714 | Wang JunYi,Jiang ManLing,Xiong AnYing,et al. Integrated Analysis of Single-Cell and Bulk RNA Sequencing Reveals Pro-Fibrotic PLA2G7(High) Macrophages in Pulmonary Fibrosis[J]. PHARMACOLOGICAL RESEARCH, 2022, 182, 106286. |
APA | Wang JunYi., Jiang ManLing., Xiong AnYing., Zhang Lei., LuoLi., LiuYao., Liu ShengBin., Ran Qin., Wu DeHong., Xiong Ying., He Xiang., Leung Elaine Lai Han., & Li GuoPing (2022). Integrated Analysis of Single-Cell and Bulk RNA Sequencing Reveals Pro-Fibrotic PLA2G7(High) Macrophages in Pulmonary Fibrosis. PHARMACOLOGICAL RESEARCH, 182, 106286. |
MLA | Wang JunYi,et al."Integrated Analysis of Single-Cell and Bulk RNA Sequencing Reveals Pro-Fibrotic PLA2G7(High) Macrophages in Pulmonary Fibrosis".PHARMACOLOGICAL RESEARCH 182(2022):106286. |
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