Glycoproteomic landscape and structural dynamics of TIM family immune checkpoints enabled by mucinase SmE

Author:

Chongsaritsinsuk Joann,Steigmeyer Alexandra D.ORCID,Mahoney Keira E.ORCID,Rosenfeld Mia A.ORCID,Lucas Taryn M.ORCID,Smith Courtney M.,Li Alice,Ince Deniz,Kearns Fiona L.,Battison Alexandria S.ORCID,Hollenhorst Marie A.,Judy Shon D.ORCID,Tiemeyer Katherine H.ORCID,Attah Victor,Kwon Catherine,Bertozzi Carolyn R.ORCID,Ferracane Michael J.ORCID,Lemmon Mark A.ORCID,Amaro Rommie E.ORCID,Malaker Stacy A.ORCID

Abstract

AbstractMucin-domain glycoproteins are densely O-glycosylated and play critical roles in a host of biological functions. In particular, the T cell immunoglobulin and mucin-domain containing family of proteins (TIM-1, -3, -4) decorate immune cells and act as key regulators in cellular immunity. However, their dense O-glycosylation remains enigmatic, primarily due to the challenges associated with studying mucin domains. Here, we demonstrate that the mucinase SmE has a unique ability to cleave at residues bearing very complex glycans. SmE enables improved mass spectrometric analysis of several mucins, including the entire TIM family. With this information in-hand, we perform molecular dynamics (MD) simulations of TIM-3 and -4 to understand how glycosylation affects structural features of these proteins. Finally, we use these models to investigate the functional relevance of glycosylation for TIM-3 function and ligand binding. Overall, we present a powerful workflow to better understand the detailed molecular structures and functions of the mucinome.

Funder

U.S. Department of Health & Human Services | NIH | National Institute of General Medical Sciences

Publisher

Springer Science and Business Media LLC

Subject

General Physics and Astronomy,General Biochemistry, Genetics and Molecular Biology,General Chemistry,Multidisciplinary

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