PTP1B phosphatase dampens iPSC-derived neutrophil motility and antimicrobial function.
Morgan A GieseDavid A BenninTaylor J SchoenAshley N PetersonJonathan H SchropeJosh BrandHo Sun JungNancy P KellerDavid J BeebeHuy Q DinhIgor I SlukvinAnna HuttenlocherPublished in: Journal of leukocyte biology (2024)
Neutrophils are rapidly recruited to sites of infection and are critical for pathogen clearance. Therapeutic use of primary neutrophils has been limited as they have a short lifespan and are not amenable to genetic manipulation. Human induced pluripotent stem cells (iPSCs) can provide a robust source of neutrophils for infusion and are genetically tractable. However, current work has indicated that dampened intracellular signaling limits iPSC-derived neutrophil (iNeutrophil) cellular activation and antimicrobial response. Here, we show that protein tyrosine phosphatase 1B (PTP1B) inhibits intracellular signaling and dampens iNeutrophil effector function. Deletion of the PTP1B phosphatase increased PI3K and ERK signaling and was associated with increased F-actin polymerization, cell migration and phagocytosis. In contrast, other effector functions like NETosis and ROS production were reduced. PTP1B-deficient neutrophils were more responsive to A. fumigatus and displayed rapid recruitment and control of hyphal growth. Accordingly, depletion of PTP1B increased production of inflammatory factors including the neutrophil chemokine IL-8. Taken together, these findings suggest that PTP1B limits iNeutrophil motility and antimicrobial function.
Keyphrases
- induced pluripotent stem cells
- cell migration
- staphylococcus aureus
- candida albicans
- biofilm formation
- magnetic resonance
- dendritic cells
- cell death
- low dose
- signaling pathway
- cell proliferation
- endothelial cells
- gene expression
- magnetic resonance imaging
- cancer therapy
- protein kinase
- immune response
- computed tomography
- pseudomonas aeruginosa
- drug delivery
- copy number
- quantum dots
- pluripotent stem cells