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Epitope-dependent Functional Effects of Celiac Disease Autoantibodies on Transglutaminase 2.

J Biol Chem. 2016; 
Hnida K, Stamnaes J, du Pré MF, Mysling S, J?rgensen TJ, Sollid LM, Iversen R.
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Codon Optimization 5 and 679-14-D04 IgD BCR were generated by retroviral transduction as previously described for the other BCRs using codon-optimized synthetic DNA (GenScript) (12, 14) A20 cells expressing HLA-DQ2.... BCR molecules were pulled down from the supernatant by incubation with pro- tein L-agarose (GenScript) fo r 1 h at 4 °C,followed by elution with SDS-PAGE sample buffer containing 2-mercaptoethanol. Get A Quote

摘要

Transglutaminase 2 (TG2) is a Ca2+-dependent cross-linking enzyme involved in the pathogenesis of CD. We have previously characterized a panel of anti-TG2 mAbs generated from gut plasma cells of celiac patients and identified four epitopes (epitopes 1-4) located in the N-terminal part of TG2. Binding of the mAbs induced allosteric changes in TG2. Thus, we aimed to determine whether these mAbs could influence enzymatic activity through modulation of TG2 susceptibility to oxidative inactivation and Ca2+ affinity. All tested epitope 1 mAbs, as well as 679-14-D04, which recognizes a previously uncharacterized epitope, prevented oxidative inactivation and increased Ca2+ sensitivity of TG2. We have identified crucial... More

關鍵詞

allosteric regulation; antibody; autoimmunity; capillary electrophoresis; celiac disease; enzyme catalysis; hydrogen/deuterium exchange; mass spectrometry (MS); transglutaminase
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