[No authors listed]
Atopic dermatitis (AD) is a type of chronic skin inflammation and one of the most common relapsing allergic diseases, which presents with a severe rash and itchy skin lesions. The pathogenesis of AD is primarily associated with hyperâactivated mast cells, which makes them an effective treatment target. After crossâlinking the antigen/immunoglobulin (Ig) E complex binds to its high affinity receptor FcεRl on the surface of mast cells. The cells subsequently secrete excessive proâinflammatory mediators, including histamine and cytokines, which lead to pruritus and immune cell infiltration in the skin lesions. The present study screened natural compounds that have an inhibitory effect on IgE/antigenâmediated secretory activity. It was revealed that cryptotanshinone (CRT), a natural compound extracted from Salvia miltiorrhiza Bunge, had inhibitory effects on the IgE/antigen complex. The underlying mechanism by which CRT exerted an antiâallergy/inflammatory function was investigated using rat basophilic leukaemia (RBL) cells for degranulation assays and a 1âchloroâ2,4âdinitrobenzene (DNCB)âinduced AD Balb/c mouse model for in vivo study. CRT effectively mitigated the secretion of proâinflammatory cytokines, including tumor necrosis factorâα and interleukin 1β, as well as immune cell infiltration into skin lesions in a mouse model of ADâlike skin disease induced by dinitrochlorobenzene. The inhibitory effect of CRT on IgEâmediated mast cell degranulation was mediated by the inhibition of tyrosine kinaseâdependent degranulation signalling pathways involving spleen tyrosine kinase and Lyn. The present study revealed CRT as an inhibitor of mast cell degranulation. Therefore, CRT may be considered for development as a therapeutic drug to treat IgEâmediated skin diseases.
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