4.4 Article

MASP-1 and MASP-3 Bind Directly to Aspergillus fumigatus and Promote Complement Activation and Phagocytosis

JOURNAL OF INNATE IMMUNITY (2021)

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Journal

JOURNAL OF INNATE IMMUNITY
Volume 13, Issue 4, Pages 211-224

Publisher

KARGER
DOI: 10.1159/000514546

Keywords

Lectin pathway; Mannose-binding lectin-associated serine protease; Pattern recognition molecules; Fungi; Aspergillosis

Categories

Immunology

Funding

  1. Novo Nordisk Foundation [NNF18SA0034956]
  2. Danish Research Foundation of Independent Research [DFF6110-00489]
  3. Sven Andersen Research Foundation
  4. Novo Nordisk Research Foundation
  5. Rigshospitalet
  6. Austrian Science Funds (FWF) doctoral program Host response in opportunistic infections (HOROS) [W1253]

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Complement system activation relies on the interaction between pathogens and pattern recognition molecules, particularly through MASPs in the lectin pathway. This study found that MASPs can independently recognize certain fungal pathogens, such as the dangerous Aspergillus fumigatus, facilitating complement activation. MASPs were observed to have dual functions as enzymes and as PRMs, revealing a previously unknown pathway for complement activation.
Activation of the complement system is mediated by the interaction between pathogens and pattern recognition molecules (PRMs); mannose-binding lectin (MBL), ficolins, and collectin-10/-11 from the lectin pathway and C1q from the classical pathway. Lectin pathway activation specifically depends on proteases named MBL-associated serine proteases (MASPs) that are found in complexes with PRMs. In this study, we hypothesize that MASPs can recognize selected pathogens independently of PRMs. Using different clinical strains of opportunistic fungi, we have observed that MASPs directly recognize certain fungal pathogens in a way that can facilitate complement activation. Among these were Aspergillus fumigatus - a dangerous pathogen, especially for immunocompromised patients. In flow cytometry and fluorescence microscopy, we found that MASP-1 and -3 bound to all A. fumigatus growth stages (conidia, germ tubes, and hyphae), whereas rMASP-2 and the nonproteolytic rMAP-1 did not. Bound rMASPs could recruit rMBL and rficolin-3 to A. fumigatus conidia in a nonclassical manner and activate complement via rMASP-2. In experiments using recombinant and purified components, rMASP-1 increased the neutrophilic phagocytosis of conidia. In serum where known complement activation pathways were blocked, phagocytosis could be mediated by rMASP-3. We have encountered an unknown pathway for complement activation and found that MASP-1 and MASP-3 have dual functions as enzymes and as PRMs.

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