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19 results on '"Bogyo M"'

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1. Mixed alkyl/aryl phosphonates identify metabolic serine hydrolases as antimalarial targets.

2. Mitigating the risk of antimalarial resistance via covalent dual-subunit inhibition of the Plasmodium proteasome.

3. Identification of covalent inhibitors that disrupt M. tuberculosis growth by targeting multiple serine hydrolases involved in lipid metabolism.

4. Toxoplasma gondii serine hydrolases regulate parasite lipid mobilization during growth and replication within the host.

5. Selective activation of PFKL suppresses the phagocytic oxidative burst.

6. Strategies for Tuning the Selectivity of Chemical Probes that Target Serine Hydrolases.

7. The Clinical Drug Ebselen Attenuates Inflammation and Promotes Microbiome Recovery in Mice after Antibiotic Treatment for CDI.

8. The Antimalarial Natural Product Salinipostin A Identifies Essential α/β Serine Hydrolases Involved in Lipid Metabolism in P. falciparum Parasites.

9. Synthetic Fluorogenic Peptides Reveal Dynamic Substrate Specificity of Depalmitoylases.

10. PD-1 Inhibitory Receptor Downregulates Asparaginyl Endopeptidase and Maintains Foxp3 Transcription Factor Stability in Induced Regulatory T Cells.

11. TGF-ß Regulates Cathepsin Activation during Normal and Pathogenic Development.

12. Bifunctional Probes of Cathepsin Protease Activity and pH Reveal Alterations in Endolysosomal pH during Bacterial Infection.

13. A Bright Future for Precision Medicine: Advances in Fluorescent Chemical Probe Design and Their Clinical Application.

14. Global Analysis of Palmitoylated Proteins in Toxoplasma gondii.

15. Engineered hybrid dimers: tracking the activation pathway of caspase-7.

16. Identification of early intermediates of caspase activation using selective inhibitors and activity-based probes.

17. Cathepsin cysteine proteases are effectors of invasive growth and angiogenesis during multistage tumorigenesis.

18. A cathepsin L isoform that is devoid of a signal peptide localizes to the nucleus in S phase and processes the CDP/Cux transcription factor.

19. The human cytomegalovirus US11 gene product dislocates MHC class I heavy chains from the endoplasmic reticulum to the cytosol.

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