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1. Widespread dynamic DNA methylation in response to biotic stress

2. Histone H3K18 & H3K23 acetylation directs establishment of MLL-mediated H3K4 methylation.

3. Dual roles of histone H3 lysine-4 in antagonizing Polycomb group function and promoting target gene expression.

4. Heterochromatic 3D genome organization is directed by HP1a- and H3K9-dependent and independent mechanisms.

5. H3K18 & H3K23 acetylation directs establishment of MLL-mediated H3K4 methylation.

6. Cohesin regulation and roles in chromosome structure and function.

7. Proximity-dependent recruitment of Polycomb repressive complexes by the lncRNA Airn.

8. PDS5A and PDS5B differentially affect gene expression without altering cohesin localization across the genome.

9. Chromosomal localization of cohesin is differentially regulated by WIZ, WAPL, and G9a.

10. Functional impact of cancer-associated cohesin variants on gene expression and cellular identity.

11. A cohesin cancer mutation reveals a role for the hinge domain in genome organization and gene expression.

12. Distinct and overlapping roles of STAG1 and STAG2 in cohesin localization and gene expression in embryonic stem cells.

13. A WIZ/Cohesin/CTCF Complex Anchors DNA Loops to Define Gene Expression and Cell Identity.

15. lncRNA-Induced Spread of Polycomb Controlled by Genome Architecture, RNA Abundance, and CpG Island DNA.

16. Control of cell identity genes occurs in insulated neighborhoods in mammalian chromosomes.

17. SMC complexes link gene expression and genome architecture.

18. Multiple structural maintenance of chromosome complexes at transcriptional regulatory elements.

19. Widespread dynamic DNA methylation in response to biotic stress.

20. Functional studies and homology modeling of Msh2-Msh3 predict that mispair recognition involves DNA bending and strand separation.

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