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-Subunit Expression Leads to Photoreceptor and Bipolar Cell Degeneration
1 From the Department of Ophthalmology and Visual Science, Yale University School of Medicine, New Haven, Connecticut.
PURPOSE. To determine whether alterations in rod cGMP-gated channel function
mediate retinal degeneration, a transgenic approach in which the
subunit of the rod cGMP-gated channel is reduced by the expression of
an antisense RNA was used.
METHODS. A 890-bp fragment of the 5' mouse rod cGMP-gated channel cDNA was cloned in the antisense orientation under the control of the strong bacterial cytomegalovirus promoter. This antisense construct was used to generate transgenic mice in which the expression of the antisense transgene was measured by reverse transcriptionpolymerase chain reaction. Histologic, immunocytochemical, and TdT-dUTP terminal nick-end labeling (TUNEL) analyses were performed on control and transgenic retina sections to determine the effects of antisense expression on specific cell types.
RESULTS. The antisense RNA was able to inhibit the translation of the rod channel protein in an in vitro assay. Three transgenic mouse lines expressing the antisense construct were obtained. Molecular analyses showed that the antisense is expressed in the eye of each transgenic mouse line, where it reduces rod cGMP-gated channel RNA expression. Histologic and immunocytochemical data showed that transgenic retinas have a reduced number of photoreceptors and bipolar cells. TUNEL staining confirmed that photoreceptor and bipolar cells degenerate along an apoptotic pathway.
CONCLUSIONS. Impairment of rod cGMP-gated channel
subunit expression leads to
photoreceptor and bipolar cell degeneration. These transgenic mice are
the first model of retinal degeneration caused by an alteration in the
expression of the rod cGMP-gated channel. This model system can be used
to test therapies designed to slow or stalled retinal
degenerations.
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