Isorhodopsin Rather than Rhodopsin Mediates Rod Function in RPE65 Knock-out Mice
The chromophore of visual pigments is 11-cis-retinal and, thus, in its absence, opsin is not photosensitive and no visual function exists. However, in the RPE65 knockout (Rpe65-/-) mouse, where synthesis of 11-cis-retinal does not occur, a minimal visual response from rod photoreceptors is obtained....
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Veröffentlicht in: | Proceedings of the National Academy of Sciences - PNAS 2003-11, Vol.100 (23), p.13662-13667 |
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Zusammenfassung: | The chromophore of visual pigments is 11-cis-retinal and, thus, in its absence, opsin is not photosensitive and no visual function exists. However, in the RPE65 knockout (Rpe65-/-) mouse, where synthesis of 11-cis-retinal does not occur, a minimal visual response from rod photoreceptors is obtained. We have examined if an alternative pathway exists for cis-retinoid generation in the absence of RPE65. Cyclic-light-reared, 2-month-old Rpe65-/-mice were placed in complete darkness. No exogenous retinoids were administered. After 4 weeks, enhanced a- and b-wave amplitudes were obtained, increasing >10-fold for the a-wave and >3-fold for the b-wave as compared with cyclic-light-reared Rpe65-/-mice. Visual-pigment levels increased to$\approx\!10\>pmol$per retina, compared with no measurable pigment for cyclic-light-reared Rpe65-/-mice. The λmaxof the isolated pigment was 487 nm, characteristic for isorhodopsin. Retinoid extractions confirmed the presence of 9-cis-retinal and the absence of 11-cis-retinal. Once the Rpe65-/-mice were returned to cyclic light, within 48 h the electroretinogram function returned to levels found in Rpe65-/-mice maintained in cyclic light. This dark-mediated pathway is also operational in older animals, because 13-month-old Rpe65-/-mice kept in prolonged darkness (12 weeks) had increased isorhodopsin levels and electroretinogram a- and b-wave amplitudes. These studies demonstrate that a pathway exists in the eye for the generation of 9-cis-retinal that is independent of RPE65 and light. |
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ISSN: | 0027-8424 1091-6490 |
DOI: | 10.1073/pnas.2234461100 |