Efficient Generation, Storage, and Manipulation of Fully Flexible Pharmacophore Multiplets and Their Use in 3-D Similarity Searching

Abrahamian, Edmond J.; Fox, Peter C.; Nærum, Lars; Christensen, Inge Thøger; Thøgersen, Henning; Clark, Robert D.

doi:10.1021/ci025595r

Cited by 56 publications

(67 citation statements)

References 27 publications

Supporting

Mentioning

Contrasting

Order By: Relevance

“…In order to do this a pharmacophore was built in Phase [20] and it consisted of a central acceptor/donor pair flanked on one side of an acceptor and a hydrophobic group and on the other side by one aromatic group and one hydrophobic group (see supplementary Fig 1). A Tuplet hypothesis was then constructed using triplets [21], and used in parallel with the Phase pharmacophore to find matching compounds. The search results were used to select targeted libraries that showed a large proportion of hits in either of the searches.…”

Section: Methodsmentioning

confidence: 99%

Stable formyl peptide receptor agonists that activate the neutrophil NADPH-oxidase identified through screening of a compound library

Forsman

Kalderén

Nordin

et al. 2011

Biochemical Pharmacology

View full text Add to dashboard Cite

The neutrophil formyl peptide receptors (FPR1 and FPR2) are G-protein coupled receptors that can induce pro-inflammatory as well as anti-inflammatory activities when activated. Accordingly, these receptors may become therapeutic targets for the development of novel drugs to be used for reducing the inflammation induced injuries in asthma, rheumatoid arthritis, Alzheimer's disease, cardiovascular diseases and traumatic shock. We screened a library of more then 50 K small compounds for an ability of the compounds to induce a transient rise in intracellular Ca 2+ in cells transfected to express FPR2 (earlier called FPRL1 or the lipoxin A 4 receptor). Ten agonists hits were selected for further analysis representing different chemical series and five new together with five earlier described molecules were further profiled.. Compounds 1 -10 gave rise to a calcium response in the FPR2 transfectants with EC 50 values ranging from 4 x 10 -9 M to 2 x 10 -7 M. All 10 compounds activated human neutrophils to release superoxide , and based on the potency of their activity, the three most potent activators of the neutrophil NADPH-oxidase were further characterized. These three agonists were largely resistant to inactivation by neutrophil produced reactive oxygen species and shown to trigger the same functional repertoire in neutrophils as earlier described peptide agonists. Accordingly they induced chemotaxis, granule mobilization and secretion of superoxide. Interestingly, the oxidase activity was largely inhibited by cyclosporine H, an FPR1 selective antagonist, but not by PBP10, an FPR2 selective inhibitor, suggesting that FPR1 is the preferred receptor in neutrophils for all three agonists.

show abstract

Section: Methodsmentioning

confidence: 99%

Stable formyl peptide receptor agonists that activate the neutrophil NADPH-oxidase identified through screening of a compound library

Forsman

Kalderén

Nordin

et al. 2011

Biochemical Pharmacology

View full text Add to dashboard Cite

show abstract

“…The resulting dataset containing 999,853 molecules underwent two screening procedures: (i) a pharmacophore-based VS; and (ii) a SBVS employing four molecular docking programs. The filtered database was subjected to a flexible search using the 3D pharmacophore model and the database searching program UNITY [208]. A group of compounds matching the pharmacophore hypothesis (i.e., those assigned with the highest UNITY scores) was docked into the InhA binding site using the molecular docking program Gold.…”

Section: Discovery Of Mycobacterium Tuberculosis Inha Inhibitors Usinmentioning

confidence: 99%

Molecular Docking and Structure-Based Drug Design Strategies

et al. 2015

View full text Add to dashboard Cite

Pharmaceutical research has successfully incorporated a wealth of molecular modeling methods, within a variety of drug discovery programs, to study complex biological and chemical systems. The integration of computational and experimental strategies has been of great value in the identification and development of novel promising compounds. Broadly used in modern drug design, molecular docking methods explore the ligand conformations adopted within the binding sites of macromolecular targets. This approach also estimates the ligand-receptor binding free energy by evaluating critical phenomena involved in the intermolecular recognition process. Today, as a variety of docking algorithms are available, an understanding of the advantages and limitations of each method is of fundamental importance in the development of effective strategies and the generation of relevant results. The purpose of this review is to examine current molecular docking strategies used in drug discovery and medicinal chemistry, exploring the advances in the field and the role played by the integration of structure-and ligand-based methods.

show abstract

“…Therefore it computes the fingerprint scores to measure the shape similarity. 23 are pharmacophore VS approaches for identifying identical features through discrete point GRID of potential energy by combining 4-feature points into a form of quadruplets. Hence the quadruplets of a ligand and database are compared against the candidates from chemical database.…”

Section: -15mentioning

confidence: 99%

DUSR (Distributed Ultrafast Shape Recognition): a Hadoop Based Tool to Identify Similar Shaped Ligand Molecules

Kumari¹,

Tripathi²,

Patel³

et al. 2017

IJPER

View full text Add to dashboard Cite

Background: Identifying potential drug candidates through Ligand-based virtual screening is often associated with processing of huge amount of data and hence is a computational intensive task. Ultrafast Shape Recognition (USR) algorithm has been reported as a faster alternative for molecular shape comparison which maps the chemical structure of query ligand into its shape moment vector to find novel chemical scaffolds in chemical compound libraries. The USR algorithm however was devoid of the ability to discriminate ligand molecules according to their pharmacokinetic features. Methods: To overcome this discrepancy, a modification in the existing USR algorithm called DUSR (Distributed Ultrafast Shape Recognition) was carried out where chemical compounds were screened on the basis of their drug-likeliness properties prior to the molecular shape comparison followed by shape complementarity momentum measure. The DUSR due to its Hadoop implementation acts as a faster approach than the existing standalone tools, utilizing the MapReduce algorithm supporting the high throughput screening of million conformers in a much reduced time span. We further demonstrated the utility of DUSR on dataset of 2 million ligand molecules by running shape comparison based searching job on standalone and multisystem Hadoop platforms. Results: The result suggested that DUSR completed its job in 1h 15 m 41s, 0 h 23 m 41s and 0h13m 22s sec for 2038924 molecules on Hadoop standalone mode, 3-nodes cluster & 5-nodes cluster of distributed commodity hardware respectively.

show abstract

Efficient Generation, Storage, and Manipulation of Fully Flexible Pharmacophore Multiplets and Their Use in 3-D Similarity Searching

Cited by 56 publications

References 27 publications

Stable formyl peptide receptor agonists that activate the neutrophil NADPH-oxidase identified through screening of a compound library

Stable formyl peptide receptor agonists that activate the neutrophil NADPH-oxidase identified through screening of a compound library

Molecular Docking and Structure-Based Drug Design Strategies

DUSR (Distributed Ultrafast Shape Recognition): a Hadoop Based Tool to Identify Similar Shaped Ligand Molecules

Contact Info

Product

Resources

About