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Human cone photoreceptor dependence on RPE65 isomerase

机译:人视锥细胞感光细胞对RPE65异构酶的依赖性

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摘要

The visual (retinoid) cycle, the enzymatic pathway that regenerates chromophore after light absorption, is located primarily in the retinal pigment epithelium (RPE) and is essential for rod photoreceptor survival. Whether this pathway also is essential for cone photoreceptor survival is unknown, and there are no data from man or monkey to address this question. The visual cycle is naturally disrupted in humans with Leber congenital amaurosis (LCA), which is caused by mutations in RPE65, the gene that encodes the retinoid isomerase. We investigated such patients over a wide age range (3-52 years) for effects on the cone-rich human fovea. In vivo microscopy of the fovea showed that, even at the youngest ages, patients with RPE65-LCA exhibited cone photoreceptor loss. This loss was incomplete, however, and residual cone photoreceptor structure and function persisted for decades. Basic questions about localization of RPE65 and isomerase activity in the primate eye were addressed by examining normal macaque. RPE65 was definitively localized by immunocyto-chemistry to the central RPE and, by immunoblotting, appeared to concentrate in the central retina. The central retinal RPE layer also showed a 4-fold higher retinoid isomerase activity than more peripheral RPE. Early cone photoreceptor losses in RPE65-LCA suggest that robust RPE65-based visual chromophore production is important for cones; the residual retained cone structure and function support the speculation that alternative pathways are critical for cone photoreceptor survival.
机译:视觉(类维生素A)循环是光吸收后再生生色团的酶促途径,主要位于视网膜色素上皮(RPE)中,对于视杆感光细胞的生存至关重要。这种途径是否对视锥细胞感光器的存活也必不可少,尚无人或猴子的数据来解决这个问题。患有Leber先天性黑ama病(LCA)的人自然会破坏视力循环,这是由RPE65(编码类视黄醇异构酶的基因)中的突变引起的。我们调查了这种年龄范围较大(3-52岁)的患者对富含视锥细胞的人中央凹的影响。中央凹的体内显微镜检查显示,即使在最年轻的年龄,RPE65-LCA患者也会出现视锥细胞感光细胞丢失。然而,这种损失是不完全的,并且残留的锥体感光体的结构和功能持续了数十年。通过检查正常猕猴解决了有关RPE65的定位和灵长类动物眼睛中的异构酶活性的基本问题。 RPE65通过免疫细胞化学作用明确定位在中央RPE上,并且通过免疫印迹法似乎集中在中央视网膜上。视网膜中央RPE层还显示出比更多周边RPE高4倍的类维生素A异构酶活性。 RPE65-LCA中早期视锥光感受器的损失表明,基于RPE65的稳定生色团的产生对于视锥细胞很重要。残留的锥体结构和功能的残留支持了这样的推测,即替代途径对于锥体感光细胞的存活至关重要。

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