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1. Engineering memory T cells as a platform for long-term enzyme replacement therapy in lysosomal storage disorders.

2. Engineering Memory T Cells as a platform for Long-Term Enzyme Replacement Therapy in Lysosomal Storage Disorders.

3. Development and testing of a versatile genome editing application reporter (V-GEAR) system.

4. Precision Enhancement of CAR-NK Cells through Non-Viral Engineering and Highly Multiplexed Base Editing.

5. Generation and characterization of an immunodeficient mouse model of mucopolysaccharidosis type II.

6. Non-invasive intravenous administration of AAV9 transducing iduronate sulfatase leads to global metabolic correction and prevention of neurologic deficits in a mouse model of Hunter syndrome.

7. Neurologic Recovery in MPS I and MPS II Mice by AAV9-Mediated Gene Transfer to the CNS After the Development of Cognitive Dysfunction.

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

9. Correction of Fanconi Anemia Mutations Using Digital Genome Engineering.

10. Primary B cell engineering for therapeutic research.

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

12. Genome Engineering of Primary Human B Cells Using CRISPR/Cas9.

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

14. CRISPR/Cas9-Mediated Genome Engineering of Primary Human B Cells.

15. ZFN-Mediated In Vivo Genome Editing Corrects Murine Hurler Syndrome.

16. Engineering of Primary Human B cells with CRISPR/Cas9 Targeted Nuclease.

17. Dose-Dependent Prevention of Metabolic and Neurologic Disease in Murine MPS II by ZFN-Mediated In Vivo Genome Editing.

18. Prevention of Neurocognitive Deficiency in Mucopolysaccharidosis Type II Mice by Central Nervous System-Directed, AAV9-Mediated Iduronate Sulfatase Gene Transfer.

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