Identification of global inhibitors of cellular glycosylation

Author:

Sørensen Daniel MadrizORCID,Büll Christian,Madsen Thomas D.ORCID,Lira-Navarrete Erandi,Clausen Thomas Mandel,Clark Alex E.ORCID,Garretson Aaron F.,Karlsson RichardORCID,Pijnenborg Johan F. A.ORCID,Yin Xin,Miller Rebecca L.ORCID,Chanda Sumit K.,Boltje Thomas J.,Schjoldager Katrine T.ORCID,Vakhrushev Sergey Y.ORCID,Halim Adnan,Esko Jeffrey D.,Carlin Aaron F.ORCID,Hurtado-Guerrero RamonORCID,Weigert RobertoORCID,Clausen HenrikORCID,Narimatsu YoshikiORCID

Abstract

AbstractSmall molecule inhibitors of glycosylation enzymes are valuable tools for dissecting glycan functions and potential drug candidates. Screening for inhibitors of glycosyltransferases are mainly performed by in vitro enzyme assays with difficulties moving candidates to cells and animals. Here, we circumvent this by employing a cell-based screening assay using glycoengineered cells expressing tailored reporter glycoproteins. We focused on GalNAc-type O-glycosylation and selected the GalNAc-T11 isoenzyme that selectively glycosylates endocytic low-density lipoprotein receptor (LDLR)-related proteins as targets. Our screen of a limited small molecule compound library did not identify selective inhibitors of GalNAc-T11, however, we identify two compounds that broadly inhibited Golgi-localized glycosylation processes. These compounds mediate the reversible fragmentation of the Golgi system without affecting secretion. We demonstrate how these inhibitors can be used to manipulate glycosylation in cells to induce expression of truncated O-glycans and augment binding of cancer-specific Tn-glycoprotein antibodies and to inhibit expression of heparan sulfate and binding and infection of SARS-CoV-2.

Funder

Danmarks Grundforskningsfond

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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