Elucidating the Binding Mode between Heparin and Inflammatory Cytokines by Molecular Modeling

Dr. Mingjia Yu; Dr. Tianji Zhang; Prof. Dr. Jin‐ping Li; Prof. Dr. Yingxia Tan

doi:10.1002/open.202100135

ChemistryOpen (Oct 2021)

Elucidating the Binding Mode between Heparin and Inflammatory Cytokines by Molecular Modeling

Dr. Mingjia Yu,
Dr. Tianji Zhang,
Prof. Dr. Jin‐ping Li,
Prof. Dr. Yingxia Tan

Affiliations

Dr. Mingjia Yu: Beijing Advanced Innovation Centre for Soft Matter Science and Engineering Beijing University of Chemical Technology Beijing 100029 China
Dr. Tianji Zhang: Division of Chemistry and Analytical Science National Institute of Metrology Beijing 100029 China
Prof. Dr. Jin‐ping Li: Beijing Advanced Innovation Centre for Soft Matter Science and Engineering Beijing University of Chemical Technology Beijing 100029 China
Prof. Dr. Yingxia Tan: Department of Stem Cell and Regenerative Medicine Institute of Health Service and Transfusion Medicine Beijing 100000 China

DOI: https://doi.org/10.1002/open.202100135
Journal volume & issue: Vol. 10, no. 10
pp. 966 – 975

Abstract

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Abstract Heparan sulfate (HS) interacts with a broad spectrum of inflammatory cytokines, thereby modulating their biological activities. It is believed that there is a structural‐functional correlation between each protein and sugar sequences in the HS polysaccharides, however, the information in this regard is limited. In this study, we compared the binding of four inflammatory cytokines (CCL8, IL‐1beta, IL‐2 and IL‐6) to immobilized heparin by an SPR analysis. To define the molecular base of the binding, we used a heparin pentasaccharide as representative structure to dock into the 3D‐molecular structure of the cytokines. The results show a discrepancy in KD values obtained by SPR analysis and theoretical calculation, pointing to the importance to apply more than one method when describing affinity between proteins and HS. By cluster analysis of the complex formed between the pentasaccharide and cytokines, we have identified several groups in heparin forming strong hydrogen bonds with all four cytokines, which is a significant finding. This molecular and conformational information should be valuable for rational design of HS/heparin‐mimetics to interfere cytokine‐HS interactions.

Published in ChemistryOpen

ISSN: 2191-1363 (Online)
Publisher: Wiley-VCH
Country of publisher: Germany
LCC subjects: Science: Chemistry
Website: https://chemistry-europe.onlinelibrary.wiley.com/journal/21911363

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