Protease Inhibitors in View of Peptide Substrate Databases

Waldner, Birgit J.; Fuchs, Julian E.; Schauperl, Michael; Krämer, Christian; Liedl, Klaus R.

doi:10.1021/acs.jcim.6b00064

Cited by 4 publications

(2 citation statements)

References 32 publications

(67 reference statements)

Supporting

Mentioning

Contrasting

Order By: Relevance

“…The validation for the selected model was performed by Decoys Set Method (Keasar & Levitt, 2003; Zhou & Wishart, 2013). In which 23 best scoring adme molecules were used to search against the database of 1500 decoys generated by the online DUD-E server (Waldner, Fuchs, Schauperl, Kramer, & Liedl, 2016; Xia, Tilahun, Reid, Zhang, & Wang, 2015). The GH score method was successfully applied to quantify the selectivity of the pharmacophore model and to discover the activities from a decoy database.…”

Section: Methodsmentioning

confidence: 99%

Pharmacophore-based virtual screening of catechol-o-methyltransferase (COMT) inhibitors to combat Alzheimer’s disease

Patel

Georrge

Modi

et al. 2017

Journal of Biomolecular Structure and Dynamics

View full text Add to dashboard Cite

Alzheimer's disease (AD) is one of the most significant neurodegenerative disorders and its symptoms mostly appear in aged people. Catechol-o-methyltransferase (COMT) is one of the known target enzymes responsible for AD. With the use of 23 known inhibitors of COMT, a query has been generated and validated by screening against the database of 1500 decoys to obtain the GH score and enrichment value. The crucial features of the known inhibitors were evaluated by the online ZINC Pharmer to identify new leads from a ZINC database. Five hundred hits were retrieved from ZINC Pharmer and by ADMET (absorption, distribution, metabolism, excretion, and toxicity) filtering by using FAF-Drug-3 and 36 molecules were considered for molecular docking. From the COMT inhibitors, opicapone, fenoldopam, and quercetin were selected, while ZINC63625100_413 ZINC39411941_412, ZINC63234426_254, ZINC63637968_451, and ZINC64019452_303 were chosen for the molecular dynamics simulation analysis having high binding affinity and structural recognition. This study identified the potential COMT inhibitors through pharmacophore-based inhibitor screening leading to a more complete understanding of molecular-level interactions.

show abstract

Section: Methodsmentioning

confidence: 99%

Pharmacophore-based virtual screening of catechol-o-methyltransferase (COMT) inhibitors to combat Alzheimer’s disease

Patel

Georrge

Modi

et al. 2017

Journal of Biomolecular Structure and Dynamics

View full text Add to dashboard Cite

show abstract

“…Hence, knowledge of the substrate specificity is an important step toward understanding the biological function of a protease. Substrate specificities can be utilized for the design of active-site targeting inhibitors, as well as for the development of important research tools, such as fluorogenic substrates and activity-based probes. − Proteases recognize their substrates with pockets around the active site (called subsites), which are designated as S1–Sn at the N-terminal side of the scissile bond (nonprime side) and S1′–Sn′ at the C-terminal side of the scissile bond (prime side). The structures of these pockets allow interaction with certain amino acid side chains on the substrate, termed P sites, which have the same numbering as the subsites they occupy .…”

Section: Introductionmentioning

confidence: 99%

Protease Specificity Profiling in a Pipet Tip Using “Charge-Synchronized” Proteome-Derived Peptide Libraries

et al. 2018

View full text Add to dashboard Cite

About 2% of the genome of human and other organisms codes for proteases. An important step toward deciphering the biological function of a protease and designing inhibitors is the profiling of protease specificity. In this work we present a novel, label-free, proteomics-based protease specificity profiling method that only requires simple sample preparation steps. It uses proteome-derived peptide libraries and enriches the cleaved sequences using strong cation exchange chromatography (SCX) material in a pipet tip. As a demonstration of the method's versatility, we successfully determined the specificity of GluC, caspase-3, chymotrypsin, MMP-1 and cathepsin G from several hundreds to almost 2000 cleavage events per protease. Interestingly, we also found a novel intrinsic preference of cathepsin G for Asn at the P1 subsite, which we confirmed using synthetic peptides. Overall, this method is straightforward and requires so far the lowest investment in material and equipment for protease specificity profiling. Therefore, we think it will be applicable in any biochemistry laboratory and promote an increased understanding of protease specificity.

show abstract