323 results on '"Flotte TR"'
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2. Stable therapeutic serum levels of human alpha-1 antitrypsin (AAT) after portal vein injection of recombinant adeno-associated virus (rAAV) vectors
3. A fluorescence video-endoscopy technique for detection of gene transfer and expression
4. CFTR gene transduction in neonatal rabbits using anadeno-associated virus (AAV) vector
5. Gene Therapy 2017: Progress and Future Directions
6. Translating the genomics revolution: The need for an international gene therapy consortium for monogenic diseases
7. Cystic fibrosis transmembrane conductance regulator deficiency exacerbates islet cell dysfunction after beta-cell injury.
8. Safety and biological efficacy of an adeno-associated virus vector -- cystic fibrosis transmembrane regulator (AAV-CFTR) in the cystic fibrosis maxillary sinus.
9. Autoimmunity in a genetic disease-a cautionary tale.
10. Gene therapy in cystic fibrosis.
11. The 2024 Nobel Prize: Impact of the Discovery of miRNA on the Field of Gene Therapy.
12. The Road Less Traveled: Slow but Steady Progress Toward Cystic Fibrosis Gene Therapy by the UK Respiratory Gene Therapy Consortium.
13. Neuroimaging Applications for the Delivery and Monitoring of Gene Therapy for Central Nervous System Diseases.
14. AAV5 Delivery of CRISPR/Cas9 Mediates Genome Editing in the Lungs of Young Rhesus Monkeys.
15. Limb Perfusion Delivery of a rAAV1 Alpha-1 Antitrypsin Vector in Non-Human Primates Is Safe but Insufficient for Therapy.
16. Intrathecal gene therapy for neurologic disease in humans.
17. Kenneth I. Berns, MD, PhD [1938-2024].
18. Biodistribution and safety of a single rAAV3B-AAT vector for silencing and replacement of alpha-1 antitrypsin in Cynomolgus macaques .
19. Delivery of Adeno-Associated Virus Vectors to the Central Nervous System for Correction of Single Gene Disorders.
20. Alpha-1 Antitrypsin Deficiency.
21. Approaches to Therapeutic Gene Editing in Alpha-1 Antitrypsin Deficiency.
22. Death after High-Dose rAAV9 Gene Therapy in a Patient with Duchenne's Muscular Dystrophy. Reply.
23. Lived Experience with Gene Therapy.
24. Annual Editor's Letter.
25. Special Editorial Feature: Learning from Our Failures.
26. Immunogenicity of Recombinant Adeno-Associated Virus (AAV) Vectors for Gene Transfer.
27. Analyzing clinical observations to better understand and manage immune responses to AAV gene therapies.
28. Defining Scholarship for Today and Tomorrow.
29. Nicholas Muzyczka, PhD.
30. Gene therapy for alpha-1 antitrypsin deficiency: an update.
31. Future Directions and Resource Needs for National Heart, Lung, and Blood Institute (NHLBI) Gene Therapy Research: A Report of an NHLBI Workshop.
32. Nicholas Muzyczka, PhD [1947-2023].
33. ESGCT 2022: The New Normal for the Gene Therapy Community.
34. Secretion of functional α1-antitrypsin is cell type dependent: Implications for intramuscular delivery for gene therapy.
35. Gene Therapy for Endocrine Disorders: A Promising Intervention.
36. Gene-based therapeutics for rare genetic neurodevelopmental psychiatric disorders.
37. Gene Therapy and the Use of Animal Models: Why Mice Alone Are Not Sufficient.
38. Liver-directed SERPINA1 gene therapy attenuates progression of spontaneous and tobacco smoke-induced emphysema in α1-antitrypsin null mice.
39. Gene Therapy for Rare Neurological Disorders.
40. AAV gene therapy for Tay-Sachs disease.
41. Precision of Exon Skipping with U7 Constructs.
42. Modulating immune responses to AAV by expanded polyclonal T-regs and capsid specific chimeric antigen receptor T-regulatory cells.
43. ESGCT 2021: Virtually Pan-European.
44. In vivo gene editing works in humans: Results of a phase 1 clinical trial for TTR amyloidosis.
45. Immune Responses to Recombinant Adenoviruses As Gene Therapy Vectors and COVID-19 Vaccines: A Two-Edged Sword.
46. Base Editing to the Rescue.
47. Gene Therapy in Global Health: Meeting the Needs of Chinese Patients with Beta-Thalassemia.
48. It Is Time to Call Anti-Asian Bias What It Is: Racism.
49. Supporting Families Considering Participation in a Clinical Trial: Parent-Provider Perspectives.
50. In Reply to Ramotshwana et al.
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