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Early Alteration of Retinal Neurons in <i>Aipl1</i> <sup>?/?</sup> Animals

DOI:10.1167/iovs.13-13728 期刊:Investigative Opthalmology & Visual Science 出版年份:2014 更新时间:2025-09-23 15:22:29
摘要: PURPOSE. Mutations in the photoreceptor cell-specific gene encoding aryl hydrocarbon receptor-interacting protein-like 1 (AIPL1) lead to Leber congenital amaurosis (LCA4), retinitis pigmentosa, and cone–rod dystrophy. Gene therapy appears to be promising in the treatment for AIPL1-mediated vision loss in humans. Prior to initiating these treatments, however, it is crucial to understand how the retinal neurons remodel themselves in response to photoreceptor cell degeneration. In this study, using an animal model for AIPL1-LCA, Aipl1(cid:2)/(cid:2) mice, we investigate the changes in postreceptoral retinal neurons during the course of photoreceptor cell loss. METHODS. Morphology of the Aipl1(cid:2)/(cid:2) retina from postnatal day 8 to 150 was compared to that of age-matched, wild-type C57Bl6/J retina (WT) by immunocytochemistry using cell-specific markers. RESULTS. Expression of postsynaptic proteins in bipolar cells is reduced prior to photoreceptor cell degeneration at postnatal day 8. Bipolar and horizontal cells retract their dendrites. Cell bodies and axons of bipolar and horizontal cells are disorganized during the course of degeneration. M¨uller cell processes become hypertrophic and form a dense fibrotic layer outside the inner nuclear layer. CONCLUSIONS. An early defect in photoreceptor cells in the AIPL1-LCA mouse model affects the expression of postsynaptic markers, suggesting abnormal development of bipolar synapses. Once degeneration of photoreceptor cells is initiated, remodeling of retinal neurons in the Aipl1(cid:2)/(cid:2) animal is rapid.
作者: Ratnesh Kumar Singh,Saravanan Kolandaivelu,Visvanathan Ramamurthy
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To investigate the changes in postreceptoral retinal neurons during photoreceptor cell loss in Aipl1(cid:2)/(cid:2) mice, an animal model for AIPL1-LCA, to understand retinal remodeling for potential gene therapy applications.

The AIPL1-LCA mouse model shows early defects in photoreceptor-bipolar synapses and rapid remodeling of retinal neurons, including retraction of dendrites, disorganization of cell bodies, and glial changes, which could impact the efficacy of gene therapy and other treatments.

The study is limited to a mouse model, which may not fully replicate human conditions. Ultrastructural studies are needed to confirm synaptic abnormalities, and the exact mechanisms behind bipolar cell survival differences are not fully understood.

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