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1. Ordered and deterministic cancer genome evolution after p53 loss

2. Clonal populations of a human TNBC model display significant functional heterogeneity and divergent growth dynamics in distinct contexts

3. MACHETE identifies interferon-encompassing chromosome 9p21.3 deletions as mediators of immune evasion and metastasis

4. Mcm2 hypomorph leads to acute leukemia or hematopoietic stem cell failure, dependent on genetic context

5. Phase and context shape the function of composite oncogenic mutations

6. Senescence induction dictates response to chemo- and immunotherapy in preclinical models of ovarian cancer

7. BMP2/SMAD pathway activation in JAK2/p53-mutant megakaryocyte/erythroid progenitors promotes leukemic transformation

8. Disruption of the crypt niche promotes outgrowth of mutated colorectal tumor stem cells

9. ZSCAN10 expression corrects the genomic instability of iPSCs from aged donors

10. A unique mutator phenotype reveals complementary oncogenic lesions leading to acute leukemia

11. Somatic Tissue Engineering in Mouse Models Reveals an Actionable Role for WNT Pathway Alterations in Prostate Cancer Metastasis

12. Deletions linked to TP53 loss drive cancer through p53-independent mechanisms

13. α-Ketoglutarate links p53 to cell fate during tumour suppression

14. NK cell-mediated cytotoxicity contributes to tumor control by a cytostatic drug combination

15. Histone demethylase LSD1 is required for germinal center formation and BCL6-driven lymphomagenesis

16. An approach to suppress the evolution of resistance in BRAF

17. Cohesin Members Stag1 and Stag2 Display Distinct Roles in Chromatin Accessibility and Topological Control of HSC Self-Renewal and Differentiation

18. p53 Represses the Mevalonate Pathway to Mediate Tumor Suppression

19. Interactive analysis and assessment of single-cell copy-number variations

20. Tumor Cell-Intrinsic Factors Underlie Heterogeneity of Immune Cell Infiltration and Response to Immunotherapy

21. Transplantation of engineered organoids enables rapid generation of metastatic mouse models of colorectal cancer

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