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2. Supplementary figure S1-S7 from TAS-116, a Novel Hsp90 Inhibitor, Selectively Enhances Radiosensitivity of Human Cancer Cells to X-rays and Carbon Ion Radiation

4. Supplementary Figures 1 - 4 from Targeting the Transposase Domain of the DNA Repair Component Metnase to Enhance Chemotherapy

6. EEPD1 promotes repair of oxidatively-stressed replication forks

7. Nucleases and Co-Factors in DNA Replication Stress Responses

8. Targeting Replication Stress Response Pathways to Enhance Genotoxic Chemo- and Radiotherapy

9. Metnase and EEPD1: DNA Repair Functions and Potential Targets in Cancer Therapy

10. Recombinant cell-detecting RaDR-GFP in mice reveals an association between genomic instability and radiation-induced-thymic lymphoma

11. Exploiting DNA repair pathways for tumor sensitization, mitigation of resistance, and normal tissue protection in radiotherapy

12. The Safe Path at the Fork: Ensuring Replication-Associated DNA Double-Strand Breaks are Repaired by Homologous Recombination

13. Distinct roles of structure-specific endonucleases EEPD1 and Metnase in replication stress responses

14. Toward Greater Precision in Cancer Radiotherapy

15. Paths from DNA damage and signaling to genome rearrangements via homologous recombination

16. Mechanisms of Chromosome Translocations in Cancer

17. Endonuclease EEPD1 Is a Gatekeeper for Repair of Stressed Replication Forks

18. TAS-116, a Novel Hsp90 Inhibitor, Selectively Enhances Radiosensitivity of Human Cancer Cells to X-rays and Carbon Ion Radiation

19. The purine scaffold Hsp90 inhibitor PU-H71 sensitizes cancer cells to heavy ion radiation by inhibiting DNA repair by homologous recombination and non-homologous end joining

20. Translational research in radiation-induced DNA damage signaling and repair

21. The endonuclease EEPD1 mediates synthetic lethality in RAD52-depleted BRCA1 mutant breast cancer cells

22. Low- and High-LET Ionizing Radiation Induces Delayed Homologous Recombination that Persists for Two Weeks before Resolving

23. Clustered DNA Double-Strand Breaks: Biological Effects and Relevance to Cancer Radiotherapy

24. The DDN Catalytic Motif Is Required for Metnase Functions in Non-homologous End Joining (NHEJ) Repair and Replication Restart

25. Mechanisms of oncogenic chromosomal translocations

26. PARP1 is required for chromosomal translocations

27. Drugging the Cancers Addicted to DNA Repair

28. Targeting the Transposase Domain of the DNA Repair Component Metnase to Enhance Chemotherapy

29. Molecular basis for H3K36me3 recognition by the Tudor domain of PHF1

30. Distinct roles for DNA-PK, ATM and ATR in RPA phosphorylation and checkpoint activation in response to replication stress

31. Metnase mediates chromosome decatenation in acute leukemia cells

32. INO80-dependent chromatin remodeling regulates early and late stages of mitotic homologous recombination

33. The human set and transposase domain protein Metnase interacts with DNA Ligase IV and enhances the efficiency and accuracy of non-homologous end-joining

34. Expression levels of the human DNA repair protein metnase influence lentiviral genomic integration

35. Mechanisms of leukemia translocations

36. Distinct RAD51 Associations with RAD52 and BCCIP in Response to DNA Damage and Replication Stress

37. A YY1–INO80 complex regulates genomic stability through homologous recombination–based repair

38. BCCIP regulates homologous recombination by distinct domains and suppresses spontaneous DNA damage

39. Targeted and Nontargeted Effects of Low-Dose Ionizing Radiation on Delayed Genomic Instability in Human Cells

40. UV Radiation Induces Delayed Hyperrecombination Associated with Hypermutation in Human Cells

41. Transcription of a Donor Enhances Its Use during Double-Strand Break-Induced Gene Conversion in Human Cells

42. The SET domain protein Metnase mediates foreign DNA integration and links integration to nonhomologous end-joining repair

43. Chromatin remodelling at a DNA double-strand break site in Saccharomyces cerevisiae

44. Good Timing in the Cell Cycle for Precise DNA Repair by BRCA1

45. Gene conversion and deletion frequencies during double-strand break repair in human cells are controlled by the distance between direct repeats

46. The BRCA2-Interacting Protein BCCIP Functions in RAD51 and BRCA2 Focus Formation and Homologous Recombinational Repair

47. Characterization of palindromic loop mismatch repair tracts in mammalian cells

48. The mutagenic potential of a single DNA double-strand break in a mammalian chromosome is not influenced by transcription

49. XRCC3 Controls the Fidelity of Homologous Recombination

50. Spontaneous and double-strand break-induced recombination, and gene conversion tract lengths, are differentially affected by overexpression of wild-type or ATPase-defective yeast Rad54

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