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1. Genetic and chemical evaluation of Trypanosoma brucei oleate desaturase as a candidate drug target.

2. Fumarate hydratase isoforms of Leishmania major: Subcellular localization, structural and kinetic properties

3. Virtual Screening Identification of Nonfolate Compounds, Including a CNS Drug, as Antiparasitic Agents Inhibiting Pteridine Reductase

4. Host peroxisomal properties are not restored to normal after treatment of visceral leishmaniasis with sodium antimony gluconate

5. Peroxisome is a reservoir of intracellular calcium

6. Isolation of Leishmania glycosomes by a rapid method

7. Structure-Based Selectivity Optimization of Piperidine–Pteridine Derivatives as Potent Leishmania Pteridine Reductase Inhibitors

8. Repair of Impaired Host Peroxisomal Properties Cropped Up Due to Visceral Leishmaniasis May Lead to Overcome Peroxisome Related Genetic Disorder Which May Develop Later After Treatment

9. Stearoyl-CoA desaturase is an essential enzyme for the parasitic protist Trypanosoma brucei

10. Glucose-6-phosphate dehydrogenase of trypanosomatids: characterization, target validation, and drug discovery

11. Glucose-6-phosphate dehydrogenase is the target for the trypanocidal action of human steroids

12. Genetic and chemical evaluation of Trypanosoma brucei oleate desaturase as a candidate drug target

13. Momordicatin purified from fruits of Momordica charantia is effective to act as a potent antileishmania agent

14. An intracellular calcium store is present in Leishmania donovani glycosomes

15. Antiparasitic activity of a triphenyl tin complex against Leishmania donovani

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