Thomas B. Connor scite author profile

found in eyes with uncomplicated retinal detachments without intraocular fibrosis (360±91 pM [SEMI). Using an in vitro assay, 84-100% of the TGF-,B activity could be blocked with specific antibodies against TGF-fl2, whereas only 10-21% could be blocked by specific antibodies against TGF-,61.TGF-ft, was used in an animal model of traction retinal detachment. Since flI and 2 have essentially identical biologic effects and only human fl1 was available in quantities required, 61 was chosen for these in vivo studies. The injection of TGF-ft, plus fibronectin (FN) but not TGF-,81 alone into the vitreous cavity of rabbits resulted in the increased formation of intraocular fibrosis and traction retinal detachments as compared to control eyes. In previous studies, intravitreal FN levels were also found to be elevated in eyes with intraocular fibrosis.

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Gene therapy for red–green colour blindness in adult primates

Mancuso

Hauswirth

et al. 2009

Nature

286

218

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Red-green colour blindness, which results from the absence of either the long- (L) or middle- (M) wavelength-sensitive visual photopigments, is the most common single locus genetic disorder. Here, the possibility of curing colour blindness using gene therapy was explored in experiments on adult monkeys that had been colour blind since birth. A third type of cone pigment was added to dichromatic retinas, providing the receptoral basis for trichromatic colour vision. This opened a new avenue to explore the requirements for establishing the neural circuits for a new dimension of colour sensation. Classic visual deprivation experiments1 have led to the expectation that neural connections established during development would not appropriately process an input that was not present from birth. Therefore, it was believed that treatment of congenital vision disorders would be ineffective unless administered to the very young. Here, however, addition of a third opsin in adult red-green colour-deficient primates was sufficient to produce trichromatic colour vision behaviour. Thus, trichromacy can arise from a single addition of a third cone class and it does not require an early developmental process. This provides a positive outlook for the potential of gene therapy to cure adult vision disorders.

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Relationship Between Foveal Cone Specialization and Pit Morphology in Albinism

Wilk

McAllister

Cooper

et al. 2014

Invest. Ophthalmol. Vis. Sci.

123

159

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Progression of Geographic Atrophy in Age-related Macular Degeneration

Keenan¹,

Agrón²,

Domalpally³

et al. 2018

Ophthalmology

142

104

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Analyses of AREDS2 data on natural history of GA provide representative data on GA evolution and enlargement. GA enlargement, which was influenced by lesion features, was relentless, resulting in rapid central vision loss. The genetic variants associated with faster enlargement were partially distinct from those associated with risk of incident GA. These findings are relevant to further investigations of GA pathogenesis and clinical trial planning.

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The Effect of Cone Opsin Mutations on Retinal Structure and the Integrity of the Photoreceptor Mosaic

Carroll

Dubra

Gardner³

et al. 2012

Invest. Ophthalmol. Vis. Sci.

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The photoreceptor phenotype associated with OPN1LW and OPN1MW mutations is highly variable. These findings have implications for the potential restoration of visual function in subjects with opsin mutations. Our study highlights the importance of high-resolution phenotyping to characterize cellular structure in inherited retinal disease; such information will be critical for selecting patients most likely to respond to therapeutic intervention and for establishing a baseline for evaluating treatment efficacy.

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Thomas B. Connor

Correlation of fibrosis and transforming growth factor-beta type 2 levels in the eye.

Gene therapy for red–green colour blindness in adult primates

Relationship Between Foveal Cone Specialization and Pit Morphology in Albinism

Progression of Geographic Atrophy in Age-related Macular Degeneration

The Effect of Cone Opsin Mutations on Retinal Structure and the Integrity of the Photoreceptor Mosaic

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