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59 results on '"Joël Lelièvre"'

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1. Development of a novel secondary phenotypic screen to identify hits within the mycobacterial protein synthesis pipeline

2. Antimycobacterial drug discovery using Mycobacteria-infected amoebae identifies anti-infectives and new molecular targets

3. Prioritizing multiple therapeutic targets in parallel using automated DNA-encoded library screening

4. Identification of KasA as the cellular target of an anti-tubercular scaffold

5. Correction: Author Correction: Prioritizing multiple therapeutic targets in parallel using automated DNA-encoded library screening

6. A New Set of Chemical Starting Points with Plasmodium falciparum Transmission-Blocking Potential for Antimalarial Drug Discovery.

7. Mycobacterial dihydrofolate reductase inhibitors identified using chemogenomic methods and in vitro validation.

8. Release of 50 new, drug-like compounds and their computational target predictions for open source anti-tubercular drug discovery.

9. Activity of clinically relevant antimalarial drugs on Plasmodium falciparum mature gametocytes in an ATP bioluminescence 'transmission blocking' assay.

10. The Tuberculosis Drug Accelerator at year 10: what have we learned?

11. A Leucyl-tRNA Synthetase Inhibitor with Broad-Spectrum Antimycobacterial Activity

12. Lack of Specificity of Phenotypic Screens for Inhibitors of the Mycobacterium tuberculosis FAS-II System

13. Development of a novel secondary phenotypic screen to identify hits within the mycobacterial protein synthesis pipeline

14. The multi-target aspect of an MmpL3 inhibitor: The BM212 series of compounds bind EthR2, a transcriptional regulator of ethionamide activation

15. Essential but Not Vulnerable: Indazole Sulfonamides Targeting Inosine Monophosphate Dehydrogenase as Potential Leads against Mycobacterium tuberculosis

16. A new piperidinol derivative targeting mycolic acid transport inMycobacterium abscessus

17. Development of high throughput screening methods for inhibitors of ClpC1P1P2 from Mycobacteria tuberculosis

18. High-throughput metabolomic analysis predicts mode of action of uncharacterized antimicrobial compounds

19. Accelerating Early Antituberculosis Drug Discovery by Creating Mycobacterial Indicator Strains That Predict Mode of Action

20. Failure of in vitro differentiation of Plasmodium falciparum gametocytes into ookinetes arises because of poor gamete fertilisation

21. Endoperoxide-based compounds: cross-resistance with artemisinins and selection of a Plasmodium falciparum lineage with a K13 non-synonymous polymorphism

22. A Phenotypic Based Target Screening Approach Delivers New Antitubercular CTP Synthetase Inhibitors

23. Combinations of β-Lactam Antibiotics Currently in Clinical Trials Are Efficacious in a DHP-I-Deficient Mouse Model of Tuberculosis Infection

24. Male and Female Plasmodium falciparum Mature Gametocytes Show Different Responses to Antimalarial Drugs

25. Prioritizing multiple therapeutic targets in parallel using automated DNA-encoded library screening

26. A new piperidinol derivative targeting mycolic acid transport in Mycobacterium abscessus

27. A novel validated assay to support the discovery of new anti-malarial gametocytocidal agents

28. Increased Tolerance to Artemisinin in Plasmodium falciparum Is Mediated by a Quiescence Mechanism

29. Identification of KasA as the cellular target of an anti-tubercular scaffold

30. Use of a Locked-Nucleic-Acid Oligomer in the Clamped-Probe Assay for Detection of a Minority Pfcrt K76T Mutant Population of Plasmodium falciparum

31. Thermodynamics and Kinetics in Micellar Media. Reaction of the Hydroxide Ion with 1,3,5-Trinitrobenzene in Aqueous Solutions of a Neutral Nonionic Surfactant. Effect of the Concentration of Background Electrolyte

32. A New Set of Chemical Starting Points with Plasmodium falciparum Transmission-Blocking Potential for Antimalarial Drug Discovery

33. Imaging-based high-throughput screening assay to identify new molecules with transmission-blocking potential against Plasmodium falciparum female gamete formation

34. Trioxaquines and Heme-Artemisinin Adducts Inhibit the In Vitro Formation of Hemozoin Better than Chloroquine

35. Red blood cells derived from peripheral blood and bone marrow CD34⁺ human haematopoietic stem cells are permissive to Plasmodium parasites infection

36. Étude des propriétés physico-chimiques et complexantes de quelques cyclodextrines modifiées

37. Activity of clinically relevant antimalarial drugs on plasmodium falciparum mature gametocytes in an atp bioluminescence >transmission blocking> assay

38. Evidence for the contribution of the hemozoin synthesis pathway of the murine Plasmodium yoelii to the resistance to artemisinin-related drugs

39. Redox-switched amphiphilic ionic liquid behavior in aqueous solution

40. Exploring the FL-160-CRP gene family through sequence variability of the complement regulatory protein (CRP) expressed by the trypomastigote stage of Trypanosoma cruzi

41. Sequence diversity and differential expression of Tc52 immuno-regulatory protein in Trypanosoma cruzi: potential implications in the biological variability of strains

42. Artemisinin and chloroquine: do mode of action and mechanism of resistance involve the same protagonists?

43. Trioxaquines are new antimalarial agents active on all erythrocytic forms, including gametocytes

44. Prevalence of Plasmodium falciparum cytochrome b gene mutations in isolates imported from Africa, and implications for atovaquone resistance

45. An alternative method for Plasmodium culture synchronization

46. Collaborative approaches for Target ID in neglected diseases: identifying new antimalarial targets

47. Counterion Effects in Aqueous Solutions of Cationic Surfactants: Electromotive Force Measurements and Thermodynamic Model

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