Peptidase allergen Der p 1 initiates apoptosis of epithelial cells independently of tight junction proteolysis

S.F. Baker, Y. Yin, S.K. Runswick, Geoffrey Stewart, Philip Thompson, D.R. Garrod, C. Robinson

    Research output: Contribution to journalArticlepeer-review

    32 Citations (Scopus)

    Abstract

    Loss of epithelial cell polarity, which can arise following disruption of tight junctions (TJs), is a precursor to the carefully orchestrated removal of moribund cells from epithelia in apoptosis. Ordinarily, this cycle of events has minimally disruptive effects on the function of the epithelial barrier, but some agents have been identified that induce apoptosis and promote epithelial leakiness. The allergen Der p 1 is a cysteine peptidase that cleaves TJ adhesion proteins and induces apoptosis in epithelial cells. This suggests the possibility that, at least for some inducers of apoptosis, these events might be causally linked. We report here that Der p 1 induces epithelial apoptosis before outright cell detachment and that apoptosis occurs within the same time span as increased paracellular permeability in polarized epithelial monolayers. Whilst TJ-deficient BEAS-2B cells were resistant to Der p 1-induced apoptosis, the cell line 1HAEo-, which was also TJ deficient, was sensitive to Der p 1, providing evidence against TJ proteolysis as a cause of apoptosis. To provide direct evidence, we propagated cells that normally express TJs in low calcium medium that prevented intercellular junction assembly. These cells retained full susceptibility to Der p 1, indicating that Der p 1-induced apoptosis is independent from TJ proteolysis.
    Original languageEnglish
    Pages (from-to)71-81
    JournalMolecular Membrane Biology
    Volume20
    Issue number1
    DOIs
    Publication statusPublished - 2003

    Fingerprint

    Dive into the research topics of 'Peptidase allergen Der p 1 initiates apoptosis of epithelial cells independently of tight junction proteolysis'. Together they form a unique fingerprint.

    Cite this