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1. CRISPR-Cas9 cytidine and adenosine base editing of splice-sites mediates highly-efficient disruption of proteins in primary and immortalized cells

2. Highly efficient multiplex human T cell engineering without double-strand breaks using Cas9 base editors

3. Table S2 from Implication of ZNF217 in Accelerating Tumor Development and Therapeutically Targeting ZNF217-Induced PI3K–AKT Signaling for the Treatment of Metastatic Osteosarcoma

4. Supplementary Data from Implication of ZNF217 in Accelerating Tumor Development and Therapeutically Targeting ZNF217-Induced PI3K–AKT Signaling for the Treatment of Metastatic Osteosarcoma

5. A Pan-RNase Inhibitor Enabling CRISPR-mRNA Platforms for Engineering of Primary Human Monocytes

6. Author Correction: Highly efficient multiplex human T cell engineering without double-strand breaks using Cas9 base editors

7. Implication of ZNF217 in Accelerating Tumor Development and Therapeutically Targeting ZNF217-Induced PI3K–AKT Signaling for the Treatment of Metastatic Osteosarcoma

8. Non-Viral Engineering of CAR-NK and CAR-T cells using theTc BusterTransposon System™

9. Internal checkpoint regulates T cell neoantigen reactivity and susceptibility to PD1 blockade

10. CRISPR-Cas9 cytidine and adenosine base editing of splice-sites mediates highly-efficient disruption of proteins in primary and immortalized cells

11. 333 Targeting the apical intracellular checkpoint CISH unleashes T cell neoantigen reactivity and effector program

12. 35 Targeted non-viral integration of large cargo in primary human T cells by CRISPR/Cas9 guided homology mediated end joining

13. Internal checkpoint regulates T cell neoantigen reactivity and susceptibility to PD1 blockade

14. PLX3397 treatment inhibits constitutive CSF1R-induced oncogenic ERK signaling, reduces tumor growth, and metastatic burden in osteosarcoma

15. Internal Checkpoint Regulates T Cell Neoantigen Reactivity and Susceptibility to PD1 Blockade

16. Highly efficient multiplex human T cell engineering without double-strand breaks using Cas9 base editors

17. SEMA4C is a novel target to limit osteosarcoma growth, progression, and metastasis

18. SEMA4C is a novel target to limit osteosarcoma growth, progression, and metastasis

19. CRISPR/Cas9-Based Positive Screens for Cancer-Related Traits

20. CRISPR/Cas9-Based Positive Screens for Cancer-Related Traits

21. Highly efficient multiplex human T cell engineering without double-strand breaks using Cas9 base editors

22. Dose-dependent differential mRNA target selection and regulation by let-7a-7f and miR-17-92 cluster microRNAs

23. Abstract 1097: The miR-17-92 microRNA cluster plays a crucial role in osteosarcoma progression

24. Dimethyl Fumarate Induces Cytoprotection and Inhibits Inflammation and Vaso-Occlusion in Transgenic Sickle Mice

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