Single‐cell landscape revealed immune characteristics associated with disease phases in brucellosis patients

Author:

Wang Yi1ORCID,Yang Siyuan2345,Han Bing67,Du Xiufang8,Sun Huali9,Du Yufeng8,Liu Yinli8,Lu Panpan8,Di Jinyu10,Luu Laurence Don Wai11,Lv Xiao10,Hu Songnian1213,Wang Linghang4,Jiang Rongmeng47

Affiliation:

1. Experimental Research Center, Capital Institute of Pediatrics Beijing China

2. Beijing Key Laboratory of Emerging Infectious Diseases, Institute of Infectious Diseases, Beijing Ditan Hospital Capital Medical University Beijing China

3. Beijing Institute of Infectious Diseases Beijing China

4. National Center for Infectious Diseases, Beijing Ditan Hospital Capital Medical University Beijing China

5. National Key Laboratory of Intelligent Tracking and Forecasting for Infectious Diseases Beijing China

6. Clinical and Research Center of Infectious Diseases, Beijing Ditan Hospital Capital Medical University Beijing China

7. Beijing Quality Control and Improvement Center of Infectious Disease Beijing China

8. The Department of Infectious Diseases The Third People's Hospital of Linfen City Linfen Shanxi China

9. Department of Infectious Diseases The Affiliated Hospital of Qingdao University Qingdao Shandong China

10. Department of Clinical Laboratory The Third People's Hospital of Lifen City Linfen Shanxi China

11. School of Life Sciences University of Technology Sydney Sydney Australia

12. State Key Laboratory of Microbial Resources, Institute of Microbiology Chinese Academy of Sciences Beijing China

13. University of Chinese Academy of Sciences Beijing China

Abstract

AbstractA comprehensive immune landscape for Brucella infection is crucial for developing new treatments for brucellosis. Here, we utilized single‐cell RNA sequencing (scRNA‐seq) of 290,369 cells from 35 individuals, including 29 brucellosis patients from acute (n = 10), sub‐acute (n = 9), and chronic (n = 10) phases as well as six healthy donors. Enzyme‐linked immunosorbent assays were applied for validation within this cohort. Brucella infection caused a significant change in the composition of peripheral immune cells and inflammation was a key feature of brucellosis. Acute patients are characterized by potential cytokine storms resulting from systemic upregulation of S100A8/A9, primarily due to classical monocytes. Cytokine storm may be mediated by activating S100A8/A9‐TLR4‐MyD88 signaling pathway. Moreover, monocytic myeloid‐derived suppressor cells were the probable contributors to immune paralysis in acute patients. Chronic patients are characterized by a dysregulated Th1 response, marked by reduced expression of IFN‐γ and Th1 signatures as well as a high exhausted state. Additionally, Brucella infection can suppress apoptosis in myeloid cells (e.g., mDCs, classical monocytes), inhibit antigen presentation in professional antigen‐presenting cells (APCs; e.g., mDC) and nonprofessional APCs (e.g., monocytes), and induce exhaustion in CD8+ T/NK cells, potentially resulting in the establishment of chronic infection. Overall, our study systemically deciphered the coordinated immune responses of Brucella at different phases of the infection, which facilitated a full understanding of the immunopathogenesis of brucellosis and may aid the development of new effective therapeutic strategies, especially for those with chronic infection.

Publisher

Wiley

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