SAR and X-ray. A New Approach Combining Fragment-Based Screening and Rational Drug Design:  Application to the Discovery of Nanomolar Inhibitors of Src SH2

Lesuisse, Dominique; Lange, Gudrun; Deprez, Pierre; Bénard, Didier; Schoot, Bernard; Delettre, Georges; Marquette, Jean‐Pierre; Broto, Pierre; Jean‐Baptiste, Véronique; Bichet, Paulette; Sarubbi, Edoardo; Mandine, Eliane

doi:10.1021/jm010927p

Cited by 94 publications

(84 citation statements)

References 28 publications

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“…At the same time less common PARP inhibition assay needed a validation on some known fragment inhibitors. We have chosen two known PARP inhibitors: 4-aminobenzamide (IC 50 NAD + [66]). Experimentally obtained IC 50 values were 17 and 49 μM (600 μM NAD + ) respectively, which were in good agreement with the literature data.…”

Section: The Clustering Of Vs Results and Selection Of Compounds For mentioning

confidence: 99%

Hit clustering can improve virtual fragment screening: CDK2 and PARP1 case studies

et al. 2011

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Virtual fragment screening could be a promising alternative to existing experimental screening techniques. However, reliable methods of in silico fragment screening are yet to be established and validated. In order to develop such an approach we first checked how successful the existing molecular docking methods can be in predicting fragment binding affinities and poses. Using our Lead Finder docking software the RMSD of the binding energy prediction was observed to be 1.35 kcal/mol(-1) on a set of 26 experimentally characterized fragment inhibitors, and the RMSD of the predicted binding pose from the experimental one was <1.5 Å. Then, we explored docking of 68 fragments obtained from 39 drug molecules for which co-crystal structures were available from the PDB. It appeared that fragments that participate in oriented non-covalent interactions, such as hydrogen bonds and metal coordination, could be correctly docked in 70-80% of cases suggesting the potential success of rediscovering of corresponding drugs by in silico fragment approach. Based on these findings we've developed a virtual fragment screening technique which involved structural filtration of protein-ligand complexes for specific interactions and subsequent clustering in order to minimize the number of preferable starting fragment candidates. Application of this method led to 2 millimolar-scale fragment PARP1 inhibitors with a new scaffold.

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Section: The Clustering Of Vs Results and Selection Of Compounds For mentioning

confidence: 99%

Hit clustering can improve virtual fragment screening: CDK2 and PARP1 case studies

et al. 2011

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“…Therefore, if the compounds entering the lead discovery process are already too drug-like, the lead optimisation process will further increase MW and lipophilicity, potentially reducing the drug-like properties. Fragmentbased screening (Lesuisse et al 2002;Carr and Hann 2002;Rees et al 2004) employs significantly smaller and functionally simpler compounds, the advantage being that with fewer compounds a more efficient evaluation of the chemical space is achieved leading to a more rapid hit-to-lead optimisation phase. The downside, however, is that these fragments tend to have very low potencies (millimolar) and may be difficult to detect in standard assay systems.…”

Section: Target Identification and Validationmentioning

confidence: 99%

The challenges of developing novel antiparasitic drugs

Woods

Williams

2007

Invert Neurosci

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Only a few novel classes of antiparasitic drugs have emerged over the last few decades, reflecting the difficulties associated with bringing a safe, effective molecule to market. In recent years, the screening paradigm has shifted from empirical whole parasite screening towards mechanism-based high throughput screening. This approach requires investment in molecular parasitology and in understanding the basic biology of parasites, as well as requiring considerable investment in an infrastructure for screening. Add to this the fact that the drug discovery process is iterative with high attrition, the Animal Health industry by necessity must focus on discovering medicines for diseases, which will deliver a return on investment. In recent years the rapid progression of genomics has unlocked a plethora of tools for target identification, validation and screening, revolutionising mechanism-based screening for antiparasitic drug discovery. The challenge still remains; however, to identify novel chemical entities with the properties required to deliver a safe, effective antiparasitic drug.

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“…Until now, osteoporosis has generally been treated with two categories of drugs: bone resorption inhibitors such as biphosphonate, and stimulants of bone formation, such as parathyroid hormone and prostaglandin E2 [216]. In recent years several pharmaceutical companies including Glaxo, ARIAD and Aventis have been working to develop Src SH2 inhibitors, with the rationale that Src is a validated therapeutic target for bone resorption [178,217,218].…”

Section: Src Inhibition and Bone Resorptionmentioning

confidence: 99%

Probing the Tyrosine Phosphorylation State in Breast Cancer by Src Homology 2 Domain Binding

Mayer¹

2004

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Pubhc reporting burden for Ms collection of information is estimated to average 1 hour per response, Including the lime for reviewing instructions, searching existing data sources gathering and maintaininn the data neededI andcompletingland renewing this collection of information. Send comments regarding this burden estimate or any other asped of this collection of InfoirnaBorf iffsSÄto" educing this burden to Washington Headquarters AUTHOR(S)Bruce J. Mayer PERFORMING ORGANIZATION NAME(S) AND ADDRESS(ES)University Abstract (Maximum 200 Words) (abstract should contain no proprietary or confidential information)Improved molecular diagnostic methods that can classify tumors and predict their response to therapy have enormous potential to improve the effectiveness breast cancer treatments. The overall goal of this project is to develop a novel molecular diagnostic method, i: termed SH2 profiling, that can classify cell samples based on their global protein tyrosine phosphorylation state. The first aim is to use an existing SH2 profiling method, based on far-Western blotting, to analyze fresh surgical breast cancer samples. The second aim is to o develop a more high-throughput quantitative reversed-phase SH2 profiling format, and test its usefulness in classifying breast cancer samples. The third aim is to develop histochemical SH2 profiling methods that can be used to analyze archived, formalin-fixed tissue sections, and perform pilot retrospective studies to determine whether SH2 binding patterns have potential prognostic value. In the past year we have made great progress in developing the reversed-phase array and histochemical SH2 profiling formats, and results suggest that these quantitative methods will be useful in classifying breast cancer samples. In the coming year, once HSRRB approval for use of human samples is secured, we will begin to apply these new methods to the analysis of actual breast cancer specimens. SUBJECT TERMS Conclusions 9References 10 Appendices 10-93Mayer, B.J. INTRODUCTIONThe focus is this study is to test whether a novel molecular diagnostic approach, SH2 profiling, can serve as a useful prognostic tool to classify breast cancer. SH2 domains are small protein modules that bind specifically to tyrosine phosphorylated peptides. These domains play an important role in normal signal transduction, mediating the formation of multiprotein complexes in response to changes in tyrosine phosphorylation [1,2]. There are ~116 SH2 domains in the human genome, and different SH2 domains recognize different tyrosine phosphorylated proteins. SH2 profiling is a method in which a battery SH2 domain probes is used to provide a snapshot of the global state of tyrosine phosphorylation in a cell sample [3,4]. Different breast cancers are likely to have different patterns of tyrosine phosphorylation, reflecting differences in the signal transduction pathways active in the tumor, and thus SH2 profiling has the potential to provide a biologically relevant means to classify these tumors. In this project we prop...

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SAR and X-ray. A New Approach Combining Fragment-Based Screening and Rational Drug Design: Application to the Discovery of Nanomolar Inhibitors of Src SH2

Cited by 94 publications

References 28 publications

Hit clustering can improve virtual fragment screening: CDK2 and PARP1 case studies

Hit clustering can improve virtual fragment screening: CDK2 and PARP1 case studies

The challenges of developing novel antiparasitic drugs

Probing the Tyrosine Phosphorylation State in Breast Cancer by Src Homology 2 Domain Binding

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