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1. Lentiviral Vectors for Ocular Gene Therapy

7. Is the modification of the 13q32.1 regulatory landscape the cause of congenital microcoria?

8. Animal modelling for inherited central vision loss

10. Ophtalmologie. Thérapie génique des rétinopathies héréditaires: premiers résultats [Gene therapy for hereditary eye diseases: where are we?]

13. FAM161A, associated with retinitis pigmentosa, is a component of the cilia-basal body complex and interacts with proteins involved in ciliopathies

14. Gene therapy regenerates protein expression in cone photoreceptors in Rpe65R91W/R91W mice

16. In conditions of limited chromophore supply rods entrap 11-cis-retinal leading to loss of cone function and cell death

18. In conditions of limited chromophore supply rods entrap 11-cis-retinal leading to loss of cone function and cell death

21. In conditions of limited chromophore supply rods entrap 11-cis-retinal leading to loss of cone function and cell death

24. Adamts18 deletion results in distinct developmental defects and provides a model for congenital disorders of lens, lung, and female reproductive tract development

26. Glutamylation imbalance impairs the molecular architecture of the photoreceptor cilium.

27. PupilMetrics: a support system for preprocessing of pupillometric data and extraction of outcome measures.

28. Congenital microcoria deletion in mouse links Sox21 dysregulation to disease and suggests a role for TGFB2 in glaucoma and myopia.

29. Fine-tuning FAM161A gene augmentation therapy to restore retinal function.

30. Gene augmentation therapy attenuates retinal degeneration in a knockout mouse model of Fam161a retinitis pigmentosa.

31. Lentiviral Vectors for Ocular Gene Therapy.

32. The connecting cilium inner scaffold provides a structural foundation that protects against retinal degeneration.

33. Enhancer of Zeste Homolog 2 (EZH2) Contributes to Rod Photoreceptor Death Process in Several Forms of Retinal Degeneration and Its Activity Can Serve as a Biomarker for Therapy Efficacy.

34. Quantification of the early pupillary dilation kinetic to assess rod and cone activity.

35. A new mouse model for retinal degeneration due to Fam161a deficiency.

36. An in vitro Model of Human Retinal Detachment Reveals Successive Death Pathway Activations.

37. Lentiviral mediated RPE65 gene transfer in healthy hiPSCs-derived retinal pigment epithelial cells markedly increased RPE65 mRNA, but modestly protein level.

38. Maturation of the Pupil Light Reflex Occurs Until Adulthood in Mice.

39. Evaluation of tolerance to lentiviral LV-RPE65 gene therapy vector after subretinal delivery in non-human primates.

40. Rai1 frees mice from the repression of active wake behaviors by light.

41. Adamts18 deletion results in distinct developmental defects and provides a model for congenital disorders of lens, lung, and female reproductive tract development.

42. Amyloid Precursor-Like Protein 2 deletion-induced retinal synaptopathy related to congenital stationary night blindness: structural, functional and molecular characteristics.

43. Determination of Rod and Cone Influence to the Early and Late Dynamic of the Pupillary Light Response.

44. Animal modelling for inherited central vision loss.

45. Multigenic lentiviral vectors for combined and tissue-specific expression of miRNA- and protein-based antiangiogenic factors.

46. Notch signaling in the pigmented epithelium of the anterior eye segment promotes ciliary body development at the expense of iris formation.

47. Rapid cohort generation and analysis of disease spectrum of large animal model of cone dystrophy.

48. FAM161A, associated with retinitis pigmentosa, is a component of the cilia-basal body complex and interacts with proteins involved in ciliopathies.

49. Reduction of choroidal neovascularization in mice by adeno-associated virus-delivered anti-vascular endothelial growth factor short hairpin RNA.

50. Gene therapy regenerates protein expression in cone photoreceptors in Rpe65(R91W/R91W) mice.

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