Gene therapy restores vision in rd1 mice after removal of a confounding mutation in Gpr179

Koji M Nishiguchi; Livia S Carvalho; Matteo Rizzi; Kate Powell; Sophia-Martha kleine Holthaus; Selina A Azam; Yanai Duran; Joana Ribeiro; Ulrich F O Luhmann; James W B Bainbridge; Alexander J Smith; Robin R Ali

doi:10.1038/ncomms7006

Gene therapy restores vision in rd1 mice after removal of a confounding mutation in Gpr179

Koji M Nishiguchi, Livia S Carvalho, Matteo Rizzi, Kate Powell, Sophia-Martha kleine Holthaus, Selina A Azam, Yanai Duran, Joana Ribeiro, Ulrich F O Luhmann, James W B Bainbridge, Alexander J Smith, Robin R Ali

Research output: Contribution to journal › Article › peer-review

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Abstract

The rd1 mouse with a mutation in the Pde6b gene was the first strain of mice identified with a retinal degeneration. However, AAV-mediated gene supplementation of rd1 mice only results in structural preservation of photoreceptors, and restoration of the photoreceptor-mediated a-wave, but not in restoration of the bipolar cell-mediated b-wave. Here we show that a mutation in Gpr179 prevents the full restoration of vision in rd1 mice. Backcrossing rd1 with C57BL6 mice reveals the complete lack of b-wave in a subset of mice, consistent with an autosomal recessive Mendelian inheritance pattern. We identify a mutation in the Gpr179 gene, which encodes for a G-protein coupled receptor localized to the dendrites of ON-bipolar cells. Gene replacement in rd1 mice that are devoid of the mutation in Gpr179 successfully restores the function of both photoreceptors and bipolar cells, which is maintained for up to 13 months. Our discovery may explain the failure of previous gene therapy attempts in rd1 mice, and we propose that Grp179 mutation status should be taken into account in future studies involving rd1 mice.

Original language	English
Article number	7006
Journal	Nature Communications
Volume	6
DOIs	https://doi.org/10.1038/ncomms7006
Publication status	Published - Feb 2015
Externally published	Yes

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title = "Gene therapy restores vision in rd1 mice after removal of a confounding mutation in Gpr179",

abstract = "The rd1 mouse with a mutation in the Pde6b gene was the first strain of mice identified with a retinal degeneration. However, AAV-mediated gene supplementation of rd1 mice only results in structural preservation of photoreceptors, and restoration of the photoreceptor-mediated a-wave, but not in restoration of the bipolar cell-mediated b-wave. Here we show that a mutation in Gpr179 prevents the full restoration of vision in rd1 mice. Backcrossing rd1 with C57BL6 mice reveals the complete lack of b-wave in a subset of mice, consistent with an autosomal recessive Mendelian inheritance pattern. We identify a mutation in the Gpr179 gene, which encodes for a G-protein coupled receptor localized to the dendrites of ON-bipolar cells. Gene replacement in rd1 mice that are devoid of the mutation in Gpr179 successfully restores the function of both photoreceptors and bipolar cells, which is maintained for up to 13 months. Our discovery may explain the failure of previous gene therapy attempts in rd1 mice, and we propose that Grp179 mutation status should be taken into account in future studies involving rd1 mice.",

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author = "Nishiguchi, {Koji M} and Carvalho, {Livia S} and Matteo Rizzi and Kate Powell and Holthaus, {Sophia-Martha kleine} and Azam, {Selina A} and Yanai Duran and Joana Ribeiro and Luhmann, {Ulrich F O} and Bainbridge, {James W B} and Smith, {Alexander J} and Ali, {Robin R}",

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doi = "10.1038/ncomms7006",

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journal = "Nature Communications",

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T1 - Gene therapy restores vision in rd1 mice after removal of a confounding mutation in Gpr179

AU - Nishiguchi, Koji M

AU - Carvalho, Livia S

AU - Rizzi, Matteo

AU - Powell, Kate

AU - Holthaus, Sophia-Martha kleine

AU - Azam, Selina A

AU - Duran, Yanai

AU - Ribeiro, Joana

AU - Luhmann, Ulrich F O

AU - Bainbridge, James W B

AU - Smith, Alexander J

AU - Ali, Robin R

PY - 2015/2

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N2 - The rd1 mouse with a mutation in the Pde6b gene was the first strain of mice identified with a retinal degeneration. However, AAV-mediated gene supplementation of rd1 mice only results in structural preservation of photoreceptors, and restoration of the photoreceptor-mediated a-wave, but not in restoration of the bipolar cell-mediated b-wave. Here we show that a mutation in Gpr179 prevents the full restoration of vision in rd1 mice. Backcrossing rd1 with C57BL6 mice reveals the complete lack of b-wave in a subset of mice, consistent with an autosomal recessive Mendelian inheritance pattern. We identify a mutation in the Gpr179 gene, which encodes for a G-protein coupled receptor localized to the dendrites of ON-bipolar cells. Gene replacement in rd1 mice that are devoid of the mutation in Gpr179 successfully restores the function of both photoreceptors and bipolar cells, which is maintained for up to 13 months. Our discovery may explain the failure of previous gene therapy attempts in rd1 mice, and we propose that Grp179 mutation status should be taken into account in future studies involving rd1 mice.

AB - The rd1 mouse with a mutation in the Pde6b gene was the first strain of mice identified with a retinal degeneration. However, AAV-mediated gene supplementation of rd1 mice only results in structural preservation of photoreceptors, and restoration of the photoreceptor-mediated a-wave, but not in restoration of the bipolar cell-mediated b-wave. Here we show that a mutation in Gpr179 prevents the full restoration of vision in rd1 mice. Backcrossing rd1 with C57BL6 mice reveals the complete lack of b-wave in a subset of mice, consistent with an autosomal recessive Mendelian inheritance pattern. We identify a mutation in the Gpr179 gene, which encodes for a G-protein coupled receptor localized to the dendrites of ON-bipolar cells. Gene replacement in rd1 mice that are devoid of the mutation in Gpr179 successfully restores the function of both photoreceptors and bipolar cells, which is maintained for up to 13 months. Our discovery may explain the failure of previous gene therapy attempts in rd1 mice, and we propose that Grp179 mutation status should be taken into account in future studies involving rd1 mice.

KW - Animals

KW - Crosses, Genetic

KW - Cyclic Nucleotide Phosphodiesterases, Type 6

KW - Dependovirus

KW - Electroretinography

KW - Fear

KW - Female

KW - Fundus Oculi

KW - Genetic Therapy

KW - Genotype

KW - Homozygote

KW - Humans

KW - Male

KW - Mice

KW - Mice, Inbred C3H

KW - Mice, Inbred C57BL

KW - Mice, Transgenic

KW - Models, Genetic

KW - Mutation

KW - Plasmids

KW - Receptors, G-Protein-Coupled

KW - Retinal Degeneration

KW - Time Factors

KW - Tomography, Optical Coherence

KW - Journal Article

KW - Research Support, Non-U.S. Gov't

U2 - 10.1038/ncomms7006

DO - 10.1038/ncomms7006

M3 - Article

C2 - 25613321

SN - 2041-1723

VL - 6

JO - Nature Communications

JF - Nature Communications

M1 - 7006

ER -

Gene therapy restores vision in rd1 mice after removal of a confounding mutation in Gpr179

Abstract

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