Search

Your search keyword '"Loi, Elena M"' showing total 5 results
Start Over Author "Loi, Elena M"
5 results on '"Loi, Elena M"'

1. Discovery of a New Drug-like Series of OGT Inhibitors by Virtual Screening

Author

Loi, Elena M, Tomašič, Tihomir, Balsollier, Cyril, van Eekelen, Kevin, Weiss, Matjaž, Gobec, Martina, Alteen, Matthew G, Vocadlo, David J, Pieters, Roland J, Anderluh, Marko, Afd Chemical Biology and Drug Discovery, Chemical Biology and Drug Discovery, Afd Chemical Biology and Drug Discovery, and Chemical Biology and Drug Discovery

Subjects
Pharmaceutical Science, Farmacevtska kemija, N-Acetylglucosaminyltransferases, Analytical Chemistry, Structure-Activity Relationship, udc:615.4:54, Drug Discovery, Humans, virtualno rešetanje, Physical and Theoretical Chemistry, udc:615.4, zaviralci OGT, O-GlcNAc transferaza, Research, O-GlcNAc transferase, OGT inhibitors, virtual screening, Organic Chemistry, virtual screening, pharmaceutical chemistry, O-GlcNAc transferase, OGT inhibitors, Chemistry (miscellaneous), farmacevtska kemija, Molecular Medicine, O-GlcNAc transferaza, zaviralci OGT, virtualno rešetanje, Protein Processing, Post-Translational
Abstract

O-GlcNAcylation is an essential post-translational modification installed by the enzyme O-β-N-acetyl-d-glucosaminyl transferase (OGT). Modulating this enzyme would be extremely valuable to better understand its role in the development of serious human pathologies, such as diabetes and cancer. However, the limited availability of potent and selective inhibitors hinders the validation of this potential therapeutic target. To explore new chemotypes that target the active site of OGT, we performed virtual screening of a large library of commercially available compounds with drug-like properties. We purchased samples of the most promising virtual hits and used enzyme assays to identify authentic leads. Structure-activity relationships of the best identified OGT inhibitor were explored by generating a small library of derivatives. Our best hit displays a novel uridine mimetic scaffold and inhibited the recombinant enzyme with an IC50 value of 7 µM. The current hit represents an excellent starting point for designing and developing a new set of OGT inhibitors that may prove useful for exploring the biology of OGT. Nasl. z nasl. zaslona. Opis vira z dne 21. 3. 2022. Št. članka: 1996. Bibliografija: str. 19-21. Abstract. ARRS European Union’s Horizon2020, projekt

Published
2022

2. Discovery of a New Drug-like Series of OGT Inhibitors by Virtual Screening

Author

Afd Chemical Biology and Drug Discovery, Chemical Biology and Drug Discovery, Loi, Elena M, Tomašič, Tihomir, Balsollier, Cyril, van Eekelen, Kevin, Weiss, Matjaž, Gobec, Martina, Alteen, Matthew G, Vocadlo, David J, Pieters, Roland J, Anderluh, Marko, Afd Chemical Biology and Drug Discovery, Chemical Biology and Drug Discovery, Loi, Elena M, Tomašič, Tihomir, Balsollier, Cyril, van Eekelen, Kevin, Weiss, Matjaž, Gobec, Martina, Alteen, Matthew G, Vocadlo, David J, Pieters, Roland J, and Anderluh, Marko

Published
2022

3. New Quinolinone O-GlcNAc Transferase Inhibitors Based on Fragment Growth

Author

Afd Chemical Biology and Drug Discovery, Chemical Biology and Drug Discovery, Weiss, Matjaž, Loi, Elena M, Sterle, Maša, Balsollier, Cyril, Tomašič, Tihomir, Pieters, Roland J, Gobec, Martina, Anderluh, Marko, Afd Chemical Biology and Drug Discovery, Chemical Biology and Drug Discovery, Weiss, Matjaž, Loi, Elena M, Sterle, Maša, Balsollier, Cyril, Tomašič, Tihomir, Pieters, Roland J, Gobec, Martina, and Anderluh, Marko

Published
2021

5. Discovery of a New Drug-like Series of OGT Inhibitors by Virtual Screening.

Author

Loi EM, Tomašič T, Balsollier C, van Eekelen K, Weiss M, Gobec M, Alteen MG, Vocadlo DJ, Pieters RJ, and Anderluh M

Subjects
Humans, Research, Structure-Activity Relationship, N-Acetylglucosaminyltransferases metabolism, Protein Processing, Post-Translational
Abstract

O -GlcNAcylation is an essential post-translational modification installed by the enzyme O -β- N -acetyl-d-glucosaminyl transferase (OGT). Modulating this enzyme would be extremely valuable to better understand its role in the development of serious human pathologies, such as diabetes and cancer. However, the limited availability of potent and selective inhibitors hinders the validation of this potential therapeutic target. To explore new chemotypes that target the active site of OGT, we performed virtual screening of a large library of commercially available compounds with drug-like properties. We purchased samples of the most promising virtual hits and used enzyme assays to identify authentic leads. Structure-activity relationships of the best identified OGT inhibitor were explored by generating a small library of derivatives. Our best hit displays a novel uridine mimetic scaffold and inhibited the recombinant enzyme with an IC 50 value of 7 µM. The current hit represents an excellent starting point for designing and developing a new set of OGT inhibitors that may prove useful for exploring the biology of OGT.

Published
2022
Full Text
View/download PDF

Catalog

Books, media, physical & digital resources
See catalog results