Blocking the interaction between S100A9 protein and RAGE V domain using S100A12 protein.

Blocking the interaction between S100A9 protein and RAGE V domain using S100A12 protein.

The proteins S100A9 and S100A12 are associated with the human S100 calcium-binding protein family. These proteins promote interaction with target proteins and alter their conformation when they bind to calcium ions in EF-hand motifs. The V domain of RAGE (Receptor for Advanced Glycation End products...

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Bibliographic Details
Main Authors: Revansiddha Katte, Chin Yu
Format: Article
Language:English
Published: Public Library of Science (PLoS) 2018-01-01
Series:PLoS ONE
Online Access:https://storage.googleapis.com/plos-corpus-prod/10.1371/journal.pone.0198767/1/pone.0198767.pdf?X-Goog-Algorithm=GOOG4-RSA-SHA256&X-Goog-Credential=wombat-sa%40plos-prod.iam.gserviceaccount.com%2F20210216%2Fauto%2Fstorage%2Fgoog4_request&X-Goog-Date=20210216T183045Z&X-Goog-Expires=3600&X-Goog-SignedHeaders=host&X-Goog-Signature=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Summary:The proteins S100A9 and S100A12 are associated with the human S100 calcium-binding protein family. These proteins promote interaction with target proteins and alter their conformation when they bind to calcium ions in EF-hand motifs. The V domain of RAGE (Receptor for Advanced Glycation End products) is crucial for S100A9 binding. The binding of RAGE with S100 family proteins aids in cell proliferation. In this report, we demonstrate that S100A12 protein hinders the binding of S100A9 with the RAGE V-domain. We used fluorescence and NMR spectroscopy to analyze the interaction of S100A9 with S100A12. The binary complex models of S100A9-S100A12 were developed using data obtained from 1H-15N HSQC NMR titrations and the HADDOCK program. We overlaid the complex models of S100A9-S100A12 with the same orientation of S100A9 and the RAGE V-domain. This complex showed that S100A12 protein blocks the interaction between S100A9 and the RAGE V-domain. It means S100A12 may be used as an antagonist for S100A9. The results could be favorable for developing anti-cancer drugs based on S100 family proteins.
ISSN:1932-6203

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