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Antibody discovery identifies regulatory mechanisms of protein arginine deiminase 4

Medicine and Health

Antibody discovery identifies regulatory mechanisms of protein arginine deiminase 4

X. Zhou, S. Kong, et al.

Discover the groundbreaking research conducted by Xin Zhou, Sophie Kong, and colleagues on protein arginine deiminase 4 (PAD4), uncovering its role in rheumatoid arthritis. This study reveals how functional antibodies can activate or inhibit PAD4 activity through allosteric modulation, providing new insights into enzyme regulation that could pave the way for innovative treatment approaches.

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Playback language: English
Abstract
Unlocking the potential of protein arginine deiminase 4 (PAD4) as a drug target for rheumatoid arthritis requires a deeper understanding of its regulation. In this study, we use unbiased antibody selections to identify functional antibodies capable of either activating or inhibiting PAD4 activity. Through cryogenic-electron microscopy, we characterized the structures of these antibodies in complex with PAD4 and revealed insights into their mechanisms of action. Rather than steric occlusion of the substrate-binding catalytic pocket, the antibodies modulate PAD4 activity through interactions with allosteric binding sites adjacent to the catalytic pocket. These binding events lead to either alteration of the active site conformation or the enzyme oligomeric state, resulting in modulation of PAD4 activity. Our study uses antibody engineering to reveal new mechanisms for enzyme regulation and highlights the potential of using PAD4 agonist and antagonist antibodies for studying PAD4-dependency in disease models and future therapeutic development.
Publisher
Nature Chemical Biology
Published On
Feb 02, 2024
Authors
Xin Zhou, Sophie Kong, Allison Maker, Soumya G. Remesh, Kevin K. Leung, Kliment A. Verba, James A. Wells
Tags
PAD4
rheumatoid arthritis
functional antibodies
allosteric regulation
enzyme modulation
therapeutic development
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