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5. Conserved crosstalk between histone deacetylation and H3K79 methylation generates DOT1L‐dose dependency in HDAC1‐deficient thymic lymphoma

7. List of Contributors

12. Strength is in engagement:The rise of an online scientific community during the COVID-19 pandemic

13. Epigenetics Identifier screens reveal regulators of chromatin acylation and limited specificity of acylation antibodies

16. The histone methyltransferase DOT1L prevents antigen-independent differentiation and safeguards epigenetic identity of CD8 + T cells

18. The histone methyltransferase DOT1L prevents antigen-independent differentiation and safeguards epigenetic identity of CD8+ T cells

19. Evolutionarily-conserved chromatin crosstalk generates a DOT1L-dose dependency in thymic lymphoma caused by loss of HDAC1

20. Modeling Distributive Histone Modification by Dot1 Methyltransferases: From Mechanism to Biological Insights

21. The histone methyltransferase DOT1L prevents antigen-independent differentiation and safeguards epigenetic identity of CD8+ T cells.

22. Dot1 promotes H2B ubiquitination by a methyltransferase-independent mechanism

23. Direct screening for chromatin status on DNA barcodes in yeast delineates the regulome of H3K79 methylation by Dot1

24. Flexibility in crosstalk between H2B ubiquitination and H3 methylation in vivo (Corrigendum)

25. Author response: Direct screening for chromatin status on DNA barcodes in yeast delineates the regulome of H3K79 methylation by Dot1

26. Dot1 histone methyltransferases share a distributive mechanism but have highly diverged catalytic properties

27. Dot1 histone methyltransferases share a distributive mechanism but have highly diverged catalytic properties

29. Yeast PP4 Interacts with ATR Homolog Ddc2-Mec1 and Regulates Checkpoint Signaling

30. Flexibility in crosstalk between H2B ubiquitination and H3 methylation in vivo

31. Flexibility in crosstalk between H2B ubiquitination and H3 methylation in vivo (Corrigendum)

32. Flexibility in crosstalk between H2B ubiquitination and H3 methylation in vivo

33. Flexibility in crosstalk between H2B ubiquitination and H3 methylation in vivo

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