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Exonic mutations associated with atopic dermatitis disrupt lympho-epithelial Kazal-type related inhibitor action and enhance its degradation.

Allergy. 2020; 
Ramesh K, Matta SA, Chew FT, Mok YK.
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Codon Optimization … Genes coding for D4 and D6 (codon optimised for bacterial expression vector system) were purchased from Genscript (NJ, USA) and subcloned into a pet-M plasmid using the restriction sites for BamHI and EcoRI (Figure S3) The sequence was confirmed using Big … Get A Quote

摘要

Skin desquamation is facilitated by serine proteases KLK5 and KLK7, which are tightly regulated by lympho-epithelial Kazal-type related inhibitor (LEKTI). LEKTI itself is controlled through degraded by mesotrypsin. Here, we sought to determine whether LEKTI exonic mutations associated with atopic dermatitis (AD) affect the protease inhibitory activity of LEKTI or its susceptibility to mesotrypsin degradation.,The inhibitory activities of the LEKTI domain 4 (D4) and D6 WT and AD-associated mutants on the enzyme activities of KLK5 and KLK7 were compared using fluorogenic substrates. A keratinocyte cell culture system using HaCat cells was established to assess the role of D6 WT and D386N on triggering inflammatio... More

關鍵詞

KLK5 protease; LEKTI activity; atopic dermatitis; exonic mutation; mesotrypsin degradation
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