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1. Transcriptional reprogramming by mutated IRF4 in lymphoma

4. Regulation of developmentally controlled enhancer activity by extrinsic signals in normal and malignant cells: AP-1 at the centre.

5. GPRC5C drives branched-chain amino acid metabolism in leukemogenesis.

6. Transcriptional reprogramming by mutated IRF4 in lymphoma.

7. TFEB induces mitochondrial itaconate synthesis to suppress bacterial growth in macrophages.

8. Hyaluronic acid-GPRC5C signalling promotes dormancy in haematopoietic stem cells.

9. Multilayer omics analysis reveals a non-classical retinoic acid signaling axis that regulates hematopoietic stem cell identity.

11. Chemotherapy-induced transposable elements activate MDA5 to enhance haematopoietic regeneration.

12. Identification of gene specific cis-regulatory elements during differentiation of mouse embryonic stem cells: An integrative approach using high-throughput datasets.

13. KMT9 monomethylates histone H4 lysine 12 and controls proliferation of prostate cancer cells.

14. The Co-operation of RUNX1 with LDB1, CDK9 and BRD4 Drives Transcription Factor Complex Relocation During Haematopoietic Specification.

15. Cooperative binding of AP-1 and TEAD4 modulates the balance between vascular smooth muscle and hemogenic cell fate.

16. Chromatin programming by developmentally regulated transcription factors: lessons from the study of haematopoietic stem cell specification and differentiation.

17. Dynamic Gene Regulatory Networks Drive Hematopoietic Specification and Differentiation.

18. PRC2 inhibition counteracts the culture-associated loss of engraftment potential of human cord blood-derived hematopoietic stem and progenitor cells.

19. The RUNX1-PU.1 axis in the control of hematopoiesis.

20. Polycomb protein EED is required for silencing of pluripotency genes upon ESC differentiation.

21. Inhibition of histone deacetylases by Trichostatin A leads to a HoxB4-independent increase of hematopoietic progenitor/stem cell frequencies as a result of selective survival.

22. Chromatin flow cytometry identifies changes in epigenetic cell states.

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