Neutrophils disrupt B-1a cell homeostasis by targeting Siglec-G to exacerbate sepsis

Neutrophils disrupt B-1a cell homeostasis by targeting Siglec-G to exacerbate sepsis

B-1a cells, an innate-like cell population, are crucial for pathogen defense and the regulation of inflammation through their release of natural IgM and IL-10. In sepsis, B-1a cell numbers are decreased in the peritoneal cavity as they robustly migrate to the spleen. Within the spleen, migrating B-1...

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Veröffentlicht in:Cellular & molecular immunology 2024-07, Vol.21 (7), p.707-722
Hauptverfasser: Tan, Chuyi, Reilly, Bridgette, Ma, Gaifeng, Murao, Atsushi, Jha, Alok, Aziz, Monowar, Wang, Ping
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631/250/256/1980
Antibodies
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Medical Microbiology
Microbiology
Vaccine
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container_issue 7
container_start_page 707
container_title Cellular & molecular immunology
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creator Tan, Chuyi
Reilly, Bridgette
Ma, Gaifeng
Murao, Atsushi
Jha, Alok
Aziz, Monowar
Wang, Ping
description B-1a cells, an innate-like cell population, are crucial for pathogen defense and the regulation of inflammation through their release of natural IgM and IL-10. In sepsis, B-1a cell numbers are decreased in the peritoneal cavity as they robustly migrate to the spleen. Within the spleen, migrating B-1a cells differentiate into plasma cells, leading to alterations in their original phenotype and functionality. We discovered a key player, sialic acid-binding immunoglobulin-like lectin-G (Siglec-G), which is expressed predominantly on B-1a cells and negatively regulates B-1a cell migration to maintain homeostasis. Siglec-G interacts with CXCR4/CXCL12 to modulate B-1a cell migration. Neutrophils aid B-1a cell migration via neutrophil elastase (NE)-mediated Siglec-G cleavage. Human studies revealed increased NE expression in septic patients. We identified an NE cleavage sequence in silico, leading to the discovery of a decoy peptide that protects Siglec-G, preserves peritoneal B-1a cells, reduces inflammation, and enhances sepsis survival. The role of Siglec-G in inhibiting B-1a cell migration to maintain their inherent phenotype and function is compromised by NE in sepsis, offering valuable insights into B-1a cell homeostasis. Employing a small decoy peptide to prevent NE-mediated Siglec-G cleavage has emerged as a promising strategy to sustain peritoneal B-1a cell homeostasis, alleviate inflammation, and ultimately improve outcomes in sepsis patients.
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subjects 631/250/255/1318
631/250/256/1980
Antibodies
Biomedical and Life Sciences
Biomedicine
Immunology
Medical Microbiology
Microbiology
Vaccine
title Neutrophils disrupt B-1a cell homeostasis by targeting Siglec-G to exacerbate sepsis
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