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1. Disruption of Plasmodium falciparum kinetochore proteins destabilises the nexus between the centrosome equivalent and the mitotic apparatus.

2. The molecular basis of antimalarial drug resistance in Plasmodium vivax.

3. A framework for signaling throughout the life cycle of Babesia species

4. Fussing About Fission: Defining Variety Among Mainstream and Exotic Apicomplexan Cell Division Modes

5. Plasmodium falciparum CRK4 directs continuous rounds of DNA replication during schizogony.

6. Mode of action of artemether lumefantrine (COARTEM): The sole, fixed, oral ADCC and its role in combatting multidrug resistance

7. Heterochromatin silencing and locus repositioning linked to regulation of virulence genes in Plasmodium faiciparum

8. Single cell expression and chromatin accessibility of the Toxoplasma gondii lytic cycle identifies AP2XII-8 as an essential ribosome regulon driver.

9. Disruption of Plasmodium falciparum kinetochore proteins destabilises the nexus between the centrosome equivalent and the mitotic apparatus.

10. Descriptive, Hospital-Based, 10-Year Study of Malaria Transmission in Goa, a Southwest Indian State in the Malaria Elimination Phase.

11. The essential malaria protein PfCyRPA targets glycans to invade erythrocytes.

12. Inhibition of malaria and babesiosis parasites by putative red blood cell targeting small molecules.

13. Comparative chemical genomics in Babesia species identifies the alkaline phosphatase PhoD as a determinant of antiparasitic resistance.

14. NK cell-induced damage to P.falciparum-infected erythrocytes requires ligand-specific recognition and releases parasitophorous vacuoles that are phagocytosed by monocytes in the presence of immune IgG.

15. F-erythrocytes promote Plasmodium falciparum proliferation in sickle cell disease.

16. Development of a Plasmodium vivax biobank for functional ex vivo assays.

17. A rising tide of parasite transcriptomics propels pathogen biology.

18. International Center of Excellence for Malaria Research for South Asia and Broader Malaria Research in India.

19. Diverse Malaria Presentations across National Institutes of Health South Asia International Center for Excellence in Malaria Research Sites in India.

20. The ecology and epidemiology of malaria parasitism in wild chimpanzee reservoirs.

21. Comparative single-cell transcriptional atlases of Babesia species reveal conserved and species-specific expression profiles.

23. A Malaria Parasite Cross Reveals Genetic Determinants of Plasmodium falciparum Growth in Different Culture Media.

24. Structural organization of erythrocyte membrane microdomains and their relation with malaria susceptibility.

25. The molecular basis of antimalarial drug resistance in Plasmodium vivax.

26. A framework for signaling throughout the life cycle of Babesia species.

27. Linking nutrient sensing and gene expression in Plasmodium falciparum blood-stage parasites.

28. Three Signatures of Adaptive Polymorphism Exemplified by Malaria-Associated Genes.

29. The Modular Circuitry of Apicomplexan Cell Division Plasticity.

30. Plasmodium vivax infection compromises reticulocyte stability.

32. Co-option of Plasmodium falciparum PP1 for egress from host erythrocytes.

33. Keras R-CNN: library for cell detection in biological images using deep neural networks.

34. Fussing About Fission: Defining Variety Among Mainstream and Exotic Apicomplexan Cell Division Modes.

35. Accounting for red blood cell accessibility reveals distinct invasion strategies in Plasmodium falciparum strains.

36. Plasmodium vivax transcriptional profiling of low input cryopreserved isolates through the intraerythrocytic development cycle.

37. Adaptation of Plasmodium falciparum to humans involved the loss of an ape-specific erythrocyte invasion ligand.

38. Quantitative comparative analysis of human erythrocyte surface proteins between individuals from two genetically distinct populations.

39. Generation of an immortalized erythroid progenitor cell line from peripheral blood: A model system for the functional analysis of Plasmodium spp. invasion.

40. Fetal hemoglobin does not inhibit Plasmodium falciparum growth.

41. Structure of Plasmodium falciparum Rh5-CyRPA-Ripr invasion complex.

42. Resistance to Plasmodium falciparum in sickle cell trait erythrocytes is driven by oxygen-dependent growth inhibition.

43. Bone Marrow Is a Major Parasite Reservoir in Plasmodium vivax Infection.

44. Erythrocytes lacking the Langereis blood group protein ABCB6 are resistant to the malaria parasite Plasmodium falciparum .

45. Enhanced Ex Vivo Plasmodium vivax Intraerythrocytic Enrichment and Maturation for Rapid and Sensitive Parasite Growth Assays.

46. Lysophosphatidylcholine Regulates Sexual Stage Differentiation in the Human Malaria Parasite Plasmodium falciparum.

47. Host Cell Tropism and Adaptation of Blood-Stage Malaria Parasites: Challenges for Malaria Elimination.

48. CRISPR/Cas9 knockouts reveal genetic interaction between strain-transcendent erythrocyte determinants of Plasmodium falciparum invasion.

49. Genetic Evidence for Erythrocyte Receptor Glycophorin B Expression Levels Defining a Dominant Plasmodium falciparum Invasion Pathway into Human Erythrocytes.

50. The Molecular Basis of Erythrocyte Invasion by Malaria Parasites.

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