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Your search keyword '"Tatiana Dudnakova"' showing total 22 results

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22 results on '"Tatiana Dudnakova"'

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1. Control of endothelial cell function and arteriogenesis by MEG3:EZH2 epigenetic regulation of integrin expression

2. Importance of Long Non-coding RNAs in the Development and Disease of Skeletal Muscle and Cardiovascular Lineages

3. Mapping targets for small nucleolar RNAs in yeast [version 2; referees: 5 approved]

4. Mapping targets for small nucleolar RNAs in yeast [version 1; referees: 3 approved]

5. Deducing the stage of origin of Wilms' tumours from a developmental series of Wt1-mutant mice

6. Transient Accumulation of 5-Carboxylcytosine Indicates Involvement of Active Demethylation in Lineage Specification of Neural Stem Cells

8. Histone H3K27 methyltransferase EZH2 interacts with MEG3-lncRNA to directly regulate integrin signaling and endothelial cell function

9. Systematic mapping of small nucleolar RNA targets in human cells

10. Mapping targets for small nucleolar RNAs in yeast

11. HuD is a neural enhancer of global translation acting on mTORC1-responsive genes and sponged by the Y3 small non-coding RNA

12. Transcription factor Wilms' tumor 1 regulates developmental RNAs through 3' UTR interaction

13. Methods to Identify and Validate WT1-RNA Interaction

14. Methods to Identify and Validate WT1–RNA Interaction

15. Lineage-specific distribution of high levels of genomic

16. HuD Is a Neural Translation Enhancer Acting on mTORC1-Responsive Genes and Counteracted by the Y3 Small Non-coding RNA

17. Actin: a novel interaction partner of WT1 influencing its cell dynamic properties

18. hnRNP-U directly interacts with WT1 and modulates WT1 transcriptional activation

19. Rio1 mediates ATP-dependent final maturation of 40S ribosomal subunits

20. Transient accumulation of 5-carboxylcytosine indicates involvement of active demethylation in lineage specification of neural stem cells

21. Mapping the human miRNA interactome by CLASH reveals frequent noncanonical binding

22. Deducing the stage of origin of Wilms' tumours from a developmental series of Wt1-mutant mice

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