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Glycosaminoglycans activate peptidylarginine deiminase 4 by enhancing calcium affinity

PROCEEDINGS OF THE NATIONAL ACADEMY OF SCIENCES OF THE UNITED STATES OF AMERICA. 2025-11; 
Grzegorz P. Bereta, Ewa Bielecka, Karolina Marzec, Łukasz Pijanowski, Artur P. Biela, Piotr Wilk, Marta Kamińska, Jakub Nowak, Elżbieta Wątor-Wilk, Przemysław Grudnik, Dominik Kowalczyk, Joanna Kozieł, Piotr Mydel, Marcin Poręba, Tomasz Kantyka
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Gene Synthesis Full length human PAD4 sequence (GenBank NM_012387) with N-terminal affinity Histidine tag cloned into pET16b vector was synthesized by GenScript Biotech Corporation. Subsequent mutant variants of PAD4 were also synthesized: 1. PAD4123/126/128 (R123S K126S K128S); 2. PAD4126/128/131/134/137 (K126S K128S R131S K134S R137S); Get A Quote

摘要

Rheumatoid arthritis is a chronic inflammatory disease driven by abnormal protein modifications. These include citrullination of arginine residues by the calcium-activated enzyme peptidylarginine deiminase 4 (PAD4). However, calcium in body fluids may not fully activate PAD4, suggesting the potential involvement of other activators. In this study, we investigated the ability of glycosaminoglycans (a class of negatively charged polysaccharides) to modulate PAD4 activity. We found that model glycosaminoglycans bind to the enzyme with a nanomolar affinity, increase its calcium sensitivity, and require enzyme dimerization for activation. These effects depend on the size and negative charge of the glycosaminoglycan,... More

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