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1. Interrogating Histone Acetylation and BRD4 as Mitotic Bookmarks of Transcription

2. The BET protein BRD2 cooperates with CTCF to enforce transcriptional and architectural boundaries

3. TAp73 enhances the pentose phosphate pathway and supports cell proliferation

4. A hyperactive transcriptional state marks genome reactivation at the mitosis–G1 transition

5. Molecular Basis and Consequences of the Cytochrome c-tRNA Interaction*

6. Targeting recombinant thrombomodulin fusion protein to red blood cells provides multifaceted thromboprophylaxis

7. DOT1L/KMT4 Recruitment and H3K79 Methylation Are Ubiquitously Coupled with Gene Transcription in Mammalian Cells

8. Transport capabilities of eleven gram-positive bacteria: Comparative genomic analyses

9. Erythropoiesis provides a BRD's eye view of BET protein function

10. Occupancy by key transcription factors is a more accurate predictor of enhancer activity than histone modifications or chromatin accessibility

11. Bioinformatic analyses of bacterial HPr kinase/phosphorylase homologues

12. Biochemical Characterization of Phosphoryl Transfer Involving HPr of the Phosphoenolpyruvate-Dependent Phosphotransferase System in Treponema denticola, an Organism that Lacks PTS Permeases

13. Functions of BET proteins in erythroid gene expression

14. The BET Protein BRD2 Cooperates with CTCF to Enforce a Transcriptional Boundary in Erythroid Cells

15. A Hyperactive Transcriptional State Marks Genome Reactivation during Mitotic Exit

16. Apoptotic regulation and tRNA

17. tRNA and cytochrome c in cell death and beyond

18. Abstract 486: BET protein inhibition by JQ1 blocks EWS-FLI1 activity in Ewing sarcoma

19. Dissection of BET Protein Function in a Hematopoietic Differentiation Model

20. GATA1 and the BET Family Protein Brd3 Form a Mitotic Bookmarking Complex

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