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Vertebrate visual opsin

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(Redirected from Cyanopsin)
Three-dimensional structure of bovine rhodopsin. The seven transmembrane domains are shown in varying colors. The retinal chromophore is shown in red.

Vertebrate visual opsins are a subclass of ciliary opsins and mediate vision in vertebrates. They include the opsins in human rod and cone cells. They are often abbreviated to opsin, as they were the first opsins discovered and are still the most widely studied opsins.[1]

Opsins

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Opsin refers strictly to the apoprotein (without bound retinal). When an opsin binds retinal to form a holoprotein, it is referred to as Retinylidene protein. However, the distinction is often ignored, and opsin may refer loosely to both (regardless of whether retinal is bound).

Opsins are G-protein-coupled receptors (GPCRs) and must bind retinal ⁠— typically 11-cis-retinal ⁠— in order to be photosensitive, since the retinal acts as the chromophore. When the Retinylidene protein absorbs a photon, the retinal isomerizes and is released by the opsin. The process that follows the isomerization and renewal of retinal is known as the visual cycle. Free 11-cis-retinal is photosensitive and carries its own spectral sensitivity of 380nm.[2] However, to trigger the phototransduction cascade, the process that underlies the visual signal, the retinal must be bound to an opsin when it is isomerized. The retinylidene protein has a spectral sensitivity that differs from that of free retinal and depends on the opsin sequence.

While opsins can only bind retinal, there are two forms of retinal that can act as the chromophore for vertebrate visual opsins:

Animals living on land and marine fish form their visual pigments exclusively with retinal 1. However, many freshwater fish and amphibians can also form visual pigments with retinal 2, depending on the activation of the enzyme retinal-3,4-desaturase (GO:0061899). Many of these species can switch between these chromophores during their life cycle, to adapt to a changing habitat.[3][4]

Function

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Normalised absorption spectra of the three human photopsins and of human rhodopsin (dashed). Drawn after Bowmaker and Dartnall (1980).[5] (Absorption curves do not directly reflect sensitivity spectra.)[6]

Isomerization of 11-cis-retinal into all-trans-retinal by light induces a conformational change in the protein that activates the phototransduction pathway.

Subclasses

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There are two classes of vertebrate visual opsin, differentiated by whether they are expressed in rod or cone photoreceptors.

Cone opsins

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Opsins expressed in cone cells are called cone opsins.[1] The cone opsins are called photopsins when unbound to retinal and iodopsins when bound to retinal.[1] Cone opsins mediate photopic vision (daylight). Cone opsins are further subdivided according to the spectral sensitivity of their iodopsin, namely the wavelength at which the highest light absorption is observed (λmax).[7]

Name Abbr. Cell λmax (nm) Human variant[5]
Long-wave sensitive LWS Cone 500–570 OPN1LW "red" erythrolabe (564nm)
OPN1MW "green" chlorolabe (534nm)
Short-wave sensitive 1 SWS1 Cone 355–445 OPN1SW "blue" cyanolabe (420nm)
(extinct in monotremes)
Short-wave sensitive 2 SWS2 Cone 400–470 (extinct in therian mammals)
Rhodopsin-like 2 Rh2 Cone 480–530 (Extinct in mammals)

Rod opsins

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Opsins expressed in rod cells are called rod opsins. The rod opsins are called scotopsins when unbound to retinal and rhodopsins or porphyropsins when bound to retinal (1 and 2, respectively). Rod opsins mediate scotopic vision (dim light).[8] Compared to cone opsins, the spectral sensitivity of rhodopsin is quite stable, not deviating far from 500 nm in any vertebrate.

Name Abbr. Cell λmax (nm) Human variant[5]
Scotopsin Rh1 Rod Rhodopsin: ~500
Porphyropsin: ~522[3]
RHO human rhodopsin (498nm)

Evolution

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LWS

SWS1

SWS2

Rh2

Rh1

Extant vertebrates typically have four cone opsin classes (LWS, SWS1, SWS2, and Rh2) as well as one rod opsin class (rhodopsin, Rh1), all of which were inherited from early vertebrate ancestors. These five classes of vertebrate visual opsins emerged through a series of gene duplications beginning with LWS and ending with Rh1, according to the cladogram to the right; this serves as an example of neofunctionalization. Each class has since evolved into numerous variants.[9][10] Evolutionary relationships, deduced using the amino acid sequence of the opsins, are frequently used to categorize cone opsins into their respective class.[1] Mammals lost Rh2 and SWS2 classes during the nocturnal bottleneck. Primate ancestors later developed two LWS opsins (LWS and MWS), leaving humans with 4 visual opsins in 3 classes.

History

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George Wald received the 1967 Nobel Prize in Physiology or Medicine for his experiments in the 1950s that showed the difference in absorbance by these photopsins (see image).[11]

See also

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References

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  1. ^ a b c d Terakita A (1 March 2005). "The opsins". Genome Biology. 6 (3): 213. doi:10.1186/gb-2005-6-3-213. PMC 1088937. PMID 15774036.
  2. ^ Fasick, Jeffry I.; Robinson, Phyllis R. (23 June 2016). "Adaptations of Cetacean Retinal Pigments to Aquatic Environments". Frontiers in Ecology and Evolution. 4. doi:10.3389/fevo.2016.00070.
  3. ^ a b George Wald (1939): The Porphyropsin Visual System. In: The Journal of General Physiology. Bd. 22, S. 775–794. PDF
  4. ^ Andrew T. C. Tsin & Janie M. Flores (1985): The in vivo Regeneration of Goldfish Rhodopsin and Porphyropsin. In: J. Exp. Biol. Bd. 122, S. 269–275. PMID 3723071 PDF
  5. ^ a b c Bowmaker, J K; Dartnall, H J (1 January 1980). "Visual pigments of rods and cones in a human retina". The Journal of Physiology. 298 (1): 501–511. doi:10.1113/jphysiol.1980.sp013097. PMC 1279132. PMID 7359434.
  6. ^ Stockman, Andrew; Sharpe, Lindsay T. (June 2000). "The spectral sensitivities of the middle- and long-wavelength-sensitive cones derived from measurements in observers of known genotype". Vision Research. 40 (13): 1711–1737. doi:10.1016/S0042-6989(00)00021-3. PMID 10814758. S2CID 7886523. As Fig. 11a makes clear, MSP is of little use in defining cone spectral sensitivities except close to the photopigment λmax. The large discrepancies between MSP and other estimates of cone spectral sensitivities arise because of the small signal to noise ratio of the MSP measurements.
  7. ^ Gurevich, V. V.; Gurevich, E. V. (2010-01-01), Dartt, Darlene A. (ed.), "Phototransduction: Inactivation in Cones", Encyclopedia of the Eye, Oxford: Academic Press, pp. 370–374, doi:10.1016/b978-0-12-374203-2.00190-1, ISBN 978-0-12-374203-2, retrieved 2024-05-02
  8. ^ Shichida Y, Matsuyama T (October 2009). "Evolution of opsins and phototransduction". Philosophical Transactions of the Royal Society of London. Series B, Biological Sciences. 364 (1531): 2881–2895. doi:10.1098/rstb.2009.0051. PMC 2781858. PMID 19720651.
  9. ^ Hunt DM, Carvalho LS, Cowing JA, Davies WL (October 2009). "Evolution and spectral tuning of visual pigments in birds and mammals". Philosophical Transactions of the Royal Society of London. Series B, Biological Sciences. 364 (1531): 2941–2955. doi:10.1098/rstb.2009.0044. PMC 2781856. PMID 19720655.
  10. ^ Trezise AE, Collin SP (October 2005). "Opsins: evolution in waiting". Current Biology. 15 (19): R794–R796. Bibcode:2005CBio...15.R794T. doi:10.1016/j.cub.2005.09.025. PMID 16213808.
  11. ^ The Nobel Foundation. "The Nobel Prize in Physiology or Medicine 1967". Nobelprize.org. Nobel Media AB 2014. Retrieved 12 December 2015.