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1. Disrupting MLV integrase:BET protein interaction biases integration into quiescent chromatin and delays but does not eliminate tumor activation in a MYC/Runx2 mouse model.

2. Targeting UGCG Overcomes Resistance to Lysosomal Autophagy Inhibition

3. ERK Hyperactivation Serves as a Unified Mechanism of Escape in Intrinsic and Acquired CDK4/6 Inhibitor Resistance in Acral Lentiginous Melanoma

4. Supplementary Data Tables S1-S2 from Targeting UGCG Overcomes Resistance to Lysosomal Autophagy Inhibition

5. Supplementary Data Figures S1-S5 from Targeting UGCG Overcomes Resistance to Lysosomal Autophagy Inhibition

6. Data from Targeting UGCG Overcomes Resistance to Lysosomal Autophagy Inhibition

7. Figure S6 from MFF Regulation of Mitochondrial Cell Death Is a Therapeutic Target in Cancer

8. Table S1 from MFF Regulation of Mitochondrial Cell Death Is a Therapeutic Target in Cancer

9. Supplementary Movie S1 from MFF Regulation of Mitochondrial Cell Death Is a Therapeutic Target in Cancer

10. Supplementary Figure S2 from MFF Regulation of Mitochondrial Cell Death Is a Therapeutic Target in Cancer

11. Data from MFF Regulation of Mitochondrial Cell Death Is a Therapeutic Target in Cancer

12. Supplementary Data from MFF Regulation of Mitochondrial Cell Death Is a Therapeutic Target in Cancer

14. Dasatinib Resensitizes MAPK Inhibitor Efficacy in Standard-of-Care Relapsed Melanomas

15. ERK Hyperactivation Represents a Unified Mechanism of Escape in Intrinsic and Acquired CDK4/6 Inhibitor Resistance in Acral Lentiginous Melanoma

16. Comprehensive characterization of 536 patient-derived xenograft models prioritizes candidatesfor targeted treatment

17. fMetastatic potential in clonal melanoma cells is driven by a rare, early-invading subpopulation

18. Pre-determined diversity in resistant fates emerges from homogenous cells after anti-cancer drug treatment

19. MFF Regulation of Mitochondrial Cell Death Is a Therapeutic Target in Cancer

20. Disrupting MLV integrase:BET protein interaction biases integration into quiescent chromatin and delays but does not eliminate tumor activation in a MYC/Runx2 mouse model

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