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Publication : CRALBP supports the mammalian retinal visual cycle and cone vision.

First Author  Xue Y Year  2015
Journal  J Clin Invest Volume  125
Issue  2 Pages  727-38
PubMed ID  25607845 Mgi Jnum  J:220383
Mgi Id  MGI:5634600 Doi  10.1172/JCI79651
Citation  Xue Y, et al. (2015) CRALBP supports the mammalian retinal visual cycle and cone vision. J Clin Invest 125(2):727-38
abstractText  Mutations in the cellular retinaldehyde-binding protein (CRALBP, encoded by RLBP1) can lead to severe cone photoreceptor-mediated vision loss in patients. It is not known how CRALBP supports cone function or how altered CRALBP leads to cone dysfunction. Here, we determined that deletion of Rlbp1 in mice impairs the retinal visual cycle. Mice lacking CRALBP exhibited M-opsin mislocalization, M-cone loss, and impaired cone-driven visual behavior and light responses. Additionally, M-cone dark adaptation was largely suppressed in CRALBP-deficient animals. While rearing CRALBP-deficient mice in the dark prevented the deterioration of cone function, it did not rescue cone dark adaptation. Adeno-associated virus-mediated restoration of CRALBP expression specifically in Muller cells, but not retinal pigment epithelial (RPE) cells, rescued the retinal visual cycle and M-cone sensitivity in knockout mice. Our results identify Muller cell CRALBP as a key component of the retinal visual cycle and demonstrate that this pathway is important for maintaining normal cone-driven vision and accelerating cone dark adaptation.
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