Filaggrin insufficiency renders keratinocyte-derived small extracellular vesicles capable of modulating CD1a-mediated T cell responses

Abstract: The promoting effect of FLG loss-of-function mutations on the development of atopic dermatitis (AD) signifies the role of filaggrin in the formation of a protective skin barrier; FLG mutations are also linked to asthma, food allergy and allergic rhinitis despite the absence of the protein in the affected tissues (lungs, intestines, and the majority of the nasal mucosa). AD patients suffer from chronic inflammation and recurrent skin infections; inflammation often precedes the appearance of spatially distant al… Show more

“…As for the lipid‐specific T cells, filaggrin has been documented to exert direct inhibitory action on the lipid neoantigen‐generating phospholipase A2 (PLA2) enzyme (Jarrett et al., 2016 ). Adding to that, we have very recently determined that sEV membranes themselves contain lipid antigens suitable for CD1a presentation and are capable of inducing protective and homeostatic T cell responses (Kobiela et al., 2022 ). However, filaggrin insufficient keratinocytes secrete sEVs characterised by altered lipidome which results in a bias of the CD1a‐dependent T cell responses from IFNγ‐dependent into type 2 inflammation with increased IL‐13 secretion, thus contributing to allergic inflammation.…”

Excess filaggrin in keratinocytes is removed by extracellular vesicles to prevent premature death and this mechanism can be hijacked by Staphylococcus aureus in a TLR2‐dependent fashion

“…As for the lipid‐specific T cells, filaggrin has been documented to exert direct inhibitory action on the lipid neoantigen‐generating phospholipase A2 (PLA2) enzyme (Jarrett et al., 2016 ). Adding to that, we have very recently determined that sEV membranes themselves contain lipid antigens suitable for CD1a presentation and are capable of inducing protective and homeostatic T cell responses (Kobiela et al., 2022 ). However, filaggrin insufficient keratinocytes secrete sEVs characterised by altered lipidome which results in a bias of the CD1a‐dependent T cell responses from IFNγ‐dependent into type 2 inflammation with increased IL‐13 secretion, thus contributing to allergic inflammation.…”

Excess filaggrin in keratinocytes is removed by extracellular vesicles to prevent premature death and this mechanism can be hijacked by Staphylococcus aureus in a TLR2‐dependent fashion