Genetic Reactivation of Cone Photoreceptors Restores Visual Responses in Retinitis Pigmentosa

Volker Busskamp(Médecins Sans Frontières), Jens Duebel(Friedrich Miescher Institute), D. Bálya(Friedrich Miescher Institute), Mathias Fradot(Centre National de la Recherche Scientifique), Tim J. Viney(Friedrich Miescher Institute), Sandra Siegert(Friedrich Miescher Institute), Anna C. Groner(Médecins Sans Frontières), Erik Cabuy(Friedrich Miescher Institute), Valérie Forster(Centre National de la Recherche Scientifique), Mathias W. Seeliger(University of Tübingen), Martin Biel(Center for Integrated Protein Science Munich), Peter Humphries(Trinity College Dublin), Michel Pâques(Centre National de la Recherche Scientifique), Saddek Mohand‐Saïd(Centre National de la Recherche Scientifique), Didier Trono(Médecins Sans Frontières), Karl Deisseroth(Stanford University), José‐Alain Sahel(Centre National de la Recherche Scientifique), Serge Picaud(Centre National de la Recherche Scientifique), Botond Roska(Friedrich Miescher Institute)
Science
June 25, 2010
Cited by 642Open Access
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Abstract

Retinitis pigmentosa refers to a diverse group of hereditary diseases that lead to incurable blindness, affecting two million people worldwide. As a common pathology, rod photoreceptors die early, whereas light-insensitive, morphologically altered cone photoreceptors persist longer. It is unknown if these cones are accessible for therapeutic intervention. Here, we show that expression of archaebacterial halorhodopsin in light-insensitive cones can substitute for the native phototransduction cascade and restore light sensitivity in mouse models of retinitis pigmentosa. Resensitized photoreceptors activate all retinal cone pathways, drive sophisticated retinal circuit functions (including directional selectivity), activate cortical circuits, and mediate visually guided behaviors. Using human ex vivo retinas, we show that halorhodopsin can reactivate light-insensitive human photoreceptors. Finally, we identified blind patients with persisting, light-insensitive cones for potential halorhodopsin-based therapy.


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