Proteomics

Dataset Information

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Enantioselective OTUD7B fragment discovery through chemoproteomics screening and high-throughput optimisation


ABSTRACT: Deubiquitinating enzymes (DUBs) are key regulators of cellular homeostasis, and their dysregulation is associated with several human diseases. The ovarian tumour protease (OTU) family of DUBs are biochemically well-characterised and of therapeutic interest, yet only a few tool compounds exist to study their cellular function and therapeutic potential. Here we present a chemoproteomics fragment screening platform for identifying novel DUB-specific hit matter, that combines activity-based protein profiling with high-throughput chemistry direct-to-biology optimisation to enable rapid elaboration of initial fragment hits against OTU DUBs. Applying these approaches, we identify an enantioselective fragment for OTUD7B, and validate it using chemoproteomics and biochemical DUB activity assays.

INSTRUMENT(S): timsTOF Pro 2

ORGANISM(S): Homo Sapiens (human)

TISSUE(S): Hek-293t Cell

SUBMITTER: Aini Vuorinen  

LAB HEAD: Katrin Rittinger

PROVIDER: PXD057851 | Pride | 2025-01-13

REPOSITORIES: pride

Dataset's files

Source:
Action DRS
20K_Human_Proteome_1_seq_per_gene.fasta Fasta
3707_OTUD7B.raw Raw
3707_OTUD7B_mascot_search.csv Csv
Contaminants_2022_JPR.fasta Fasta
DC2817_ELB00124_DIA_H00BP43_P05_A12_13560.d.zip Other
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