Frontiers in Cellular and Infection Microbiology (May 2021)

Von Willebrand Factor Facilitates Intravascular Dissemination of Microsporidia Encephalitozoon hellem

  • Jialing Bao,
  • Jialing Bao,
  • Biying Mo,
  • Biying Mo,
  • Guozhen An,
  • Guozhen An,
  • Jian Luo,
  • Jian Luo,
  • Mortimer Poncz,
  • Guoqing Pan,
  • Guoqing Pan,
  • Tian Li,
  • Tian Li,
  • Zeyang Zhou,
  • Zeyang Zhou,
  • Zeyang Zhou

DOI
https://doi.org/10.3389/fcimb.2021.694957
Journal volume & issue
Vol. 11

Abstract

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Microsporidia are a group of spore-forming, fungus-related pathogens that can infect both invertebrates and vertebrates including humans. The primary infection site is usually digestive tract, but systemic infections occur as well and cause damages to organs such as lung, brain, and liver. The systemic spread of microsporidia may be intravascular, requiring attachment and colonization in the presence of shear stress. Von Willebrand Factor (VWF) is a large multimeric intravascular protein and the key attachment sites for platelets and coagulation factors. Here in this study, we investigated the interactions between VWF and microsporidia Encephalitozoon hellem (E. hellem), and the modulating effects on E. hellem after VWF binding. Microfluidic assays showed that E. hellem binds to ultra-large VWF strings under shear stress. In vitro germination assay and infection assay proved that E. hellem significantly increased the rates of germination and infection, and these effects would be reversed by VWF blocking antibody. Mass spectrometry analysis further revealed that VWF-incubation altered various aspects of E. hellem including metabolic activity, levels of structural molecules, and protein maturation. Our findings demonstrated that VWF can bind microsporidia in circulation, and modulate its pathogenicity, including promoting germination and infection rate. VWF facilitates microsporidia intravascular spreading and systemic infection.

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