Unraveling transcriptomic signatures and dysregulated pathways in systemic lupus erythematosus across disease states

Wang, Frank Qingyun; Shao, Li; Dang, Xiao; Wang, Yong-Fei; Chen, Shuxiong; Liu, Zhongyi; Mao, Yujing; Jiang, Yuping; Hou, Fei; Guo, Xianghua; Li, Jian; Zhang, Lili; Sang, Yuting; Zhao, Xuan; Ma, Ruirui; Zhang, Kai; Zhang, Yanfang; Yang, Jing; Wen, Xiwu; Liu, Jiong; Wei, Wei; Zhang, Chuanpeng; Li, Weiyang; Qin, Xiao; Lei, Yao; Feng, Hong; Yang, Xingtian; She, Chun Hing; Zhang, Caicai; Su, Huidong; Chen, Xinxin; Yang, Jing; Lau, Yu Lung; Wu, Qingjun; Ban, Bo; Song, Qin; Yang, Wanling

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Article: Unraveling transcriptomic signatures and dysregulated pathways in systemic lupus erythematosus across disease states

Title	Unraveling transcriptomic signatures and dysregulated pathways in systemic lupus erythematosus across disease states
Authors	Wang, Frank Qingyun Shao, Li Dang, Xiao Wang, Yong-Fei Chen, Shuxiong Liu, Zhongyi Mao, Yujing Jiang, Yuping Hou, Fei Guo, Xianghua Li, Jian Zhang, Lili Sang, Yuting Zhao, Xuan Ma, Ruirui Zhang, Kai Zhang, Yanfang Yang, Jing Wen, Xiwu Liu, Jiong Wei, Wei Zhang, Chuanpeng Li, Weiyang Qin, Xiao Lei, Yao Feng, Hong Yang, Xingtian She, Chun Hing Zhang, Caicai Su, Huidong Chen, Xinxin Yang, Jing Lau, Yu Lung Wu, Qingjun Ban, Bo Song, Qin Yang, Wanling
Issue Date	13-May-2024
Publisher	BioMed Central
Citation	Arthritis Research and Therapy, 2024, v. 26 How to Cite? DOI: http://dx.doi.org/10.1186/s13075-024-03327-4
Abstract	Objectives: This study aims to elucidate the transcriptomic signatures and dysregulated pathways in patients with Systemic Lupus Erythematosus (SLE), with a particular focus on those persisting during disease remission. Methods: We conducted bulk RNA-sequencing of peripheral blood mononuclear cells (PBMCs) from a well-defined cohort comprising 26 remission patients meeting the Low Lupus Disease Activity State (LLDAS) criteria, 76 patients experiencing disease flares, and 15 healthy controls. To elucidate immune signature changes associated with varying disease states, we performed extensive analyses, including the identification of differentially expressed genes and pathways, as well as the construction of protein-protein interaction networks. Results: Several transcriptomic features recovered during remission compared to the active disease state, including down-regulation of plasma and cell cycle signatures, as well as up-regulation of lymphocytes. However, specific innate immune response signatures, such as the interferon (IFN) signature, and gene modules involved in chromatin structure modification, persisted across different disease states. Drug repurposing analysis revealed certain drug classes that can target these persistent signatures, potentially preventing disease relapse. Conclusion: Our comprehensive transcriptomic study revealed gene expression signatures for SLE in both active and remission states. The discovery of gene expression modules persisting in the remission stage may shed light on the underlying mechanisms of vulnerability to relapse in these patients, providing valuable insights for their treatment.
Persistent Identifier	http://hdl.handle.net/10722/345970
ISSN	1478-6354 2023 Impact Factor: 4.4 2023 SCImago Journal Rankings: 1.518

DC Field	Value	Language
dc.contributor.author	Wang, Frank Qingyun	-
dc.contributor.author	Shao, Li	-
dc.contributor.author	Dang, Xiao	-
dc.contributor.author	Wang, Yong-Fei	-
dc.contributor.author	Chen, Shuxiong	-
dc.contributor.author	Liu, Zhongyi	-
dc.contributor.author	Mao, Yujing	-
dc.contributor.author	Jiang, Yuping	-
dc.contributor.author	Hou, Fei	-
dc.contributor.author	Guo, Xianghua	-
dc.contributor.author	Li, Jian	-
dc.contributor.author	Zhang, Lili	-
dc.contributor.author	Sang, Yuting	-
dc.contributor.author	Zhao, Xuan	-
dc.contributor.author	Ma, Ruirui	-
dc.contributor.author	Zhang, Kai	-
dc.contributor.author	Zhang, Yanfang	-
dc.contributor.author	Yang, Jing	-
dc.contributor.author	Wen, Xiwu	-
dc.contributor.author	Liu, Jiong	-
dc.contributor.author	Wei, Wei	-
dc.contributor.author	Zhang, Chuanpeng	-
dc.contributor.author	Li, Weiyang	-
dc.contributor.author	Qin, Xiao	-
dc.contributor.author	Lei, Yao	-
dc.contributor.author	Feng, Hong	-
dc.contributor.author	Yang, Xingtian	-
dc.contributor.author	She, Chun Hing	-
dc.contributor.author	Zhang, Caicai	-
dc.contributor.author	Su, Huidong	-
dc.contributor.author	Chen, Xinxin	-
dc.contributor.author	Yang, Jing	-
dc.contributor.author	Lau, Yu Lung	-
dc.contributor.author	Wu, Qingjun	-
dc.contributor.author	Ban, Bo	-
dc.contributor.author	Song, Qin	-
dc.contributor.author	Yang, Wanling	-
dc.date.accessioned	2024-09-04T07:06:50Z	-
dc.date.available	2024-09-04T07:06:50Z	-
dc.date.issued	2024-05-13	-
dc.identifier.citation	Arthritis Research and Therapy, 2024, v. 26	-
dc.identifier.issn	1478-6354	-
dc.identifier.uri	http://hdl.handle.net/10722/345970	-
dc.description.abstract	<p><strong>Objectives: </strong>This study aims to elucidate the transcriptomic signatures and dysregulated pathways in patients with Systemic Lupus Erythematosus (SLE), with a particular focus on those persisting during disease remission.</p><p><strong>Methods: </strong>We conducted bulk RNA-sequencing of peripheral blood mononuclear cells (PBMCs) from a well-defined cohort comprising 26 remission patients meeting the Low Lupus Disease Activity State (LLDAS) criteria, 76 patients experiencing disease flares, and 15 healthy controls. To elucidate immune signature changes associated with varying disease states, we performed extensive analyses, including the identification of differentially expressed genes and pathways, as well as the construction of protein-protein interaction networks.</p><p><strong>Results: </strong>Several transcriptomic features recovered during remission compared to the active disease state, including down-regulation of plasma and cell cycle signatures, as well as up-regulation of lymphocytes. However, specific innate immune response signatures, such as the interferon (IFN) signature, and gene modules involved in chromatin structure modification, persisted across different disease states. Drug repurposing analysis revealed certain drug classes that can target these persistent signatures, potentially preventing disease relapse.</p><p><strong>Conclusion: </strong>Our comprehensive transcriptomic study revealed gene expression signatures for SLE in both active and remission states. The discovery of gene expression modules persisting in the remission stage may shed light on the underlying mechanisms of vulnerability to relapse in these patients, providing valuable insights for their treatment.</p>	-
dc.language	eng	-
dc.publisher	BioMed Central	-
dc.relation.ispartof	Arthritis Research and Therapy	-
dc.rights	This work is licensed under a Creative Commons Attribution-NonCommercial-NoDerivatives 4.0 International License.	-
dc.title	Unraveling transcriptomic signatures and dysregulated pathways in systemic lupus erythematosus across disease states	-
dc.type	Article	-
dc.description.nature	published_or_final_version	-
dc.identifier.doi	10.1186/s13075-024-03327-4	-
dc.identifier.volume	26	-
dc.identifier.eissn	1478-6362	-
dc.identifier.issnl	1478-6354	-

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Article: Unraveling transcriptomic signatures and dysregulated pathways in systemic lupus erythematosus across disease states

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