Chen Chunhe, Adler Leopold, Goletz Patrice, Gonzalez-Fernandez Federico, Thompson Debra A, Koutalos Yiannis
From the Departments of Ophthalmology and Neurosciences, Medical University of South Carolina, Charleston, South Carolina 29425.
the Departments of Ophthalmology and Pathology, University of Mississippi and G. V. (Sonny) Montgomery Veterans Affairs Medical Centers, Jackson, Mississippi 39216, and.
J Biol Chem. 2017 Nov 24;292(47):19356-19365. doi: 10.1074/jbc.M117.795187. Epub 2017 Sep 28.
Interphotoreceptor retinoid-binding protein (IRBP) is a specialized lipophilic carrier that binds the all- and 11- isomers of retinal and retinol, and this facilitates their transport between photoreceptors and cells in the retina. One of these retinoids, all-retinal, is released in the rod outer segment by photoactivated rhodopsin after light excitation. Following its release, all-retinal is reduced by the retinol dehydrogenase RDH8 to all-retinol in an NADPH-dependent reaction. However, all-retinal can also react with outer segment components, sometimes forming lipofuscin precursors, which after conversion to lipofuscin accumulate in the lysosomes of the retinal pigment epithelium and display cytotoxic effects. Here, we have imaged the fluorescence of all-retinol, all-retinal, and lipofuscin precursors in real time in single isolated mouse rod photoreceptors. We found that IRBP removes all-retinol from individual rod photoreceptors in a concentration-dependent manner. The rate constant for retinol removal increased linearly with IRBP concentration with a slope of 0.012 min μm IRBP also removed all-retinal, but with much less efficacy, indicating that the reduction of retinal to retinol promotes faster clearance of the photoisomerized rhodopsin chromophore. The presence of physiological IRBP concentrations in the extracellular medium resulted in lower levels of all-retinal and retinol in rod outer segments following light exposure. It also prevented light-induced lipofuscin precursor formation, but it did not remove precursors that were already present. These findings reveal an important and previously unappreciated role of IRBP in protecting the photoreceptor cells against the cytotoxic effects of accumulated all-retinal.
光感受器间类视黄醇结合蛋白(IRBP)是一种特殊的亲脂性载体,它能结合视黄醛和视黄醇的全反式异构体及11-顺式异构体,从而促进它们在光感受器和视网膜细胞之间的转运。这些类视黄醇中的一种,即全反式视黄醛,在光激发后由光激活的视紫红质在视杆细胞外段释放。释放后,全反式视黄醛在视黄醇脱氢酶RDH8的作用下,通过依赖NADPH的反应被还原为全反式视黄醇。然而,全反式视黄醛也能与外段成分发生反应,有时会形成脂褐素前体,这些前体在转化为脂褐素后会积聚在视网膜色素上皮细胞的溶酶体中,并表现出细胞毒性作用。在此,我们实时成像了单个分离的小鼠视杆光感受器中全反式视黄醇、全反式视黄醛和脂褐素前体的荧光。我们发现,IRBP以浓度依赖的方式从单个视杆光感受器中清除全反式视黄醇。视黄醇清除的速率常数随IRBP浓度呈线性增加,斜率为0.012 min⁻¹μm⁻¹。IRBP也能清除全反式视黄醛,但效率要低得多,这表明视黄醛还原为视黄醇能促进光异构化视紫红质发色团的更快清除。细胞外介质中生理浓度的IRBP会导致光照后视杆细胞外段中全反式视黄醛和视黄醇的水平降低。它还能防止光诱导的脂褐素前体形成,但不能清除已存在的前体。这些发现揭示了IRBP在保护光感受器细胞免受积累的全反式视黄醛细胞毒性作用方面的一个重要且以前未被认识到的作用。