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21 results on '"Luisa Albano"'

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1. Scalable GMP-compliant gene correction of CD4+ T cells with IDLV template functionally validated in vitro and in vivo

3. Modeling, optimization, and comparable efficacy of T cell and hematopoietic stem cell gene editing for treating hyper‐IgM syndrome

4. Data from Tumor-Initiating Cells of HER2-Positive Carcinoma Cell Lines Express the Highest Oncoprotein Levels and Are Sensitive to Trastuzumab

5. Translation on this Article from Tumor-Initiating Cells of HER2-Positive Carcinoma Cell Lines Express the Highest Oncoprotein Levels and Are Sensitive to Trastuzumab

6. Supplementary Figures S1-S6 from Tumor-Initiating Cells of HER2-Positive Carcinoma Cell Lines Express the Highest Oncoprotein Levels and Are Sensitive to Trastuzumab

7. Data from Protein Kinase Cα Determines HER2 Fate in Breast Carcinoma Cells with HER2 Protein Overexpression without Gene Amplification

11. Choice of template delivery mitigates the genotoxic risk and adverse impact of editing in human hematopoietic stem cells

12. BAR-Seq clonal tracking of gene-edited cells

13. Mobilization-based chemotherapy-free engraftment of gene-edited human hematopoietic stem cells

14. Efficient gene editing of human long-term hematopoietic stem cells validated by clonal tracking

15. Assessing Stealth and Sensed Base Editing in Human Hematopoietic Stem/Progenitor Cells

16. Towards Clinical Translation of Hematopoietic Cell Gene Editing for Treating Hyper-IgM Type 1

17. Preclinical modeling highlights the therapeutic potential of hematopoietic stem cell gene editing for correction of SCID-X1

18. Precise Gene Editing Preserves Hematopoietic Stem Cell Function following Transient p53-Mediated DNA Damage Response

19. Protein Kinase Cα Determines HER2 Fate in Breast Carcinoma Cells with HER2 Protein Overexpression without Gene Amplification

20. DNA damage in stem cells activates p21, inhibits p53, and induces symmetric self-renewing divisions

21. Modeling, optimization, and comparable efficacy of T cell and hematopoietic stem cell gene editing for treating hyper‐IgM syndrome

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