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1. Abstract IA14: Host autophagy mediates organ wasting and nutrient mobilization for tumor growth

2. Traip controls mushroom body size by suppressing mitotic defects

3. The UBR box E3 ligases Poe and Hyd are required for efficient Pericentrin degradation

4. Pericentrin is a Kinesin-1 Activator that Drives Centriole Motility

5. Pericentrin interacts with Kinesin-1 to drive centriole motility

6. Host autophagy mediates organ wasting and nutrient mobilization for tumor growth

7. Asterless is a Polo-like kinase 4 substrate that both activates and inhibits kinase activity depending on its phosphorylation state

8. Bridging centrioles and PCM in proper space and time

9. Host autophagy mediates organ wasting and nutrient mobilization for tumor growth

10. Actin dynamics and competition for myosin monomer govern the sequential amplification of myosin filaments

11. Fascetto interacting protein ensures proper cytokinesis and ploidy

12. Micro-computed tomography as a platform for exploring

13. Micro-computed tomography as a platform for exploring Drosophila development

14. Asterless is required for centriole length control and sperm development

15. An Asp–CaM complex is required for centrosome–pole cohesion and centrosome inheritance in neural stem cells

16. Sperm Head-Tail Linkage Requires Restriction of Pericentriolar Material to the Proximal Centriole End

18. A centrosomal scaffold shows some self-control

19. Same but different: pleiotropy in centrosome-related microcephaly

20. The centrosomin CM2 domain is a multi-functional binding domain with distinct cell cycle roles

21. Two Polo-like kinase 4 binding domains in Asterless perform distinct roles in regulating kinase stability

22. Taking Centrioles to the Elimination Round

23. Stu2 uses a 15-nm parallel coiled coil for kinetochore localization and concomitant regulation of the mitotic spindle

24. Drosophilapericentrin requires interaction with calmodulin for its function at centrosomes and neuronal basal bodies but not at sperm basal bodies

25. Polo-like Kinase 4 Autodestructs by Generating Its Slimb-Binding Phosphodegron

26. Organelle asymmetry for proper fitness, function, and fate

27. A centrosome interactome provides insight into organelle assembly and reveals a non-duplication role for Plk4

28. Phosphoregulation of STIM1 Leads to Exclusion of the Endoplasmic Reticulum from the Mitotic Spindle

29. Two Forkhead Transcription Factors Regulate the Division of Cardiac Progenitor Cells by a Polo-Dependent Pathway

30. Drosophila Methionine sulfoxide reductase A is not a methionine oxidase

31. Centrosome Function: Sometimes Less Is More

32. The SCFSlimb ubiquitin ligase regulates Plk4/Sak levels to block centriole reduplication

33. A Multicomponent Assembly Pathway Contributes to the Formation of Acentrosomal Microtubule Arrays in InterphaseDrosophilaCells

34. A novel GSK3-regulated APC:Axin interaction regulates Wnt signaling by driving a catalytic cycle of efficient βcatenin destruction

36. Newly Characterized Region of CP190 Associates with Microtubules and Mediates Proper Spindle Morphology in Drosophila Stem Cells

37. Autoinhibition and relief mechanism for Polo-like kinase 4

38. A yeast two-hybrid approach for probing protein–protein interactions at the centrosome

39. SV40 VP2 and VP3 Insertion into ER Membranes Is Controlled by the Capsid Protein VP1: Implications for DNA Translocation out of the ER

40. Live Imaging of Drosophila Larval Neuroblasts

41. Tubulin nucleotide status controls Sas-4-dependent pericentriolar material recruitment

42. Stable expression of fluorescently tagged proteins for studies of mitosis in mammalian cells

43. Centrosome fragments and microtubules are transported asymmetrically away from division plane in anaphase

44. Mitosis

45. Peripheral, non-centrosome-associated microtubules contribute to spindle formation in centrosome-containing cells

46. Reorganization of the microtubule array in prophase/prometaphase requires cytoplasmic dynein-dependent microtubule transport

47. Noscapine alters microtubule dynamics in living cells and inhibits the progression of melanoma

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