Lauren M. Congdon, Ph.D. - Publications
Affiliations: | 2012 | Genetic, Molecular, and Cell Biology | University of Southern California, Los Angeles, CA, United States |
Area:
Molecular Biology, Biochemistry| Year | Citation | Score | |||
|---|---|---|---|---|---|
| 2014 | Tuzon CT, Spektor T, Kong X, Congdon LM, Wu S, Schotta G, Yokomori K, Rice JC. Concerted activities of distinct H4K20 methyltransferases at DNA double-strand breaks regulate 53BP1 nucleation and NHEJ-directed repair. Cell Reports. 8: 430-8. PMID 25001286 DOI: 10.1016/J.Celrep.2014.06.013 | 0.772 | |||
| 2014 | Congdon LM, Sims JK, Tuzon CT, Rice JC. The PR-Set7 binding domain of Riz1 is required for the H4K20me1-H3K9me1 trans-tail 'histone code' and Riz1 tumor suppressor function. Nucleic Acids Research. 42: 3580-9. PMID 24423864 DOI: 10.1093/Nar/Gkt1377 | 0.774 | |||
| 2014 | Tuzon CT, Spektor TM, Congdon LM, Kong X, Cheung P, Kuo AJ, Yokomori K, Gozani O, Rice JC. Abstract LB-133: Orchestrated recruitment of histone methyltransferases to DNA double strand breaks facilitates 53BP1 binding and proficient repair Cancer Research. 74. DOI: 10.1158/1538-7445.Am2014-Lb-133 | 0.787 | |||
| 2011 | Spektor TM, Congdon LM, Veerappan CS, Rice JC. The UBC9 E2 SUMO conjugating enzyme binds the PR-Set7 histone methyltransferase to facilitate target gene repression. Plos One. 6: e22785. PMID 21829513 DOI: 10.1371/Journal.Pone.0022785 | 0.689 | |||
| 2010 | Wu S, Wang W, Kong X, Congdon LM, Yokomori K, Kirschner MW, Rice JC. Dynamic regulation of the PR-Set7 histone methyltransferase is required for normal cell cycle progression. Genes & Development. 24: 2531-42. PMID 20966048 DOI: 10.1101/Gad.1984210 | 0.747 | |||
| 2010 | Congdon LM, Houston SI, Veerappan CS, Spektor TM, Rice JC. PR-Set7-mediated monomethylation of histone H4 lysine 20 at specific genomic regions induces transcriptional repression. Journal of Cellular Biochemistry. 110: 609-19. PMID 20512922 DOI: 10.1002/Jcb.22570 | 0.522 | |||
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