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Human equivalent doses of l-DOPA rescues retinal morphology and visual function in a murine model of albinism

Human equivalent doses of l-DOPA rescues retinal morphology and visual function in a murine model of albinism
Human equivalent doses of l-DOPA rescues retinal morphology and visual function in a murine model of albinism

l-DOPA is deficient in the developing albino eye, resulting in abnormalities of retinal development and visual impairment. Ongoing retinal development after birth has also been demonstrated in the developing albino eye offering a potential therapeutic window in humans. To study whether human equivalent doses of l-DOPA/Carbidopa administered during the crucial postnatal period of neuroplasticity can rescue visual function, OCA C57BL/6 J-c2J OCA1 mice were treated with a 28-day course of oral l-DOPA/Carbidopa at 3 different doses from 15 to 43 days postnatal age (PNA) and for 3 different lengths of treatment, to identify optimum dosage and treatment length. Visual electrophysiology, acuity, and retinal morphology were measured at 4, 5, 6, 12 and 16 weeks PNA and compared to untreated C57BL/6 J (WT) and OCA1 mice. Quantification of PEDF, βIII-tubulin and syntaxin-3 expression was also performed. Our data showed impaired retinal morphology, decreased retinal function and lower visual acuity in untreated OCA1 mice compared to WT mice. These changes were diminished or eliminated when treated with higher doses of l-DOPA/Carbidopa. Our results demonstrate that oral l-DOPA/Carbidopa supplementation at human equivalent doses during the postnatal critical period of retinal neuroplasticity can rescue visual retinal morphology and retinal function, via PEDF upregulation and modulation of retinal synaptogenesis, providing a further step towards developing an effective treatment for albinism patients.

2045-2322
Sanchez-Bretano, Aida
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Keeling, Eloise
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Scott, Jennifer A.
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Lynn, Savannah A.
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Soundara-Pandi, Sudha Priya
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Macdonald, Sarah L.
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Newall, Tutte
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Griffiths, Helen
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Lotery, Andrew J.
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Ratnayaka, J. Arjuna
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Self, Jay E.
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Lee, Helena
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Sanchez-Bretano, Aida
bdbca28e-1abb-4597-856c-52f7f66d1803
Keeling, Eloise
3207bbdb-d391-44af-8abc-a60c08dce45b
Scott, Jennifer A.
bdc803de-3082-4727-a4ca-f5a1cf3fcfcc
Lynn, Savannah A.
de0c4ec2-8a3c-4b16-9e47-ea13abc32a3b
Soundara-Pandi, Sudha Priya
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Macdonald, Sarah L.
047cba55-3ca3-489d-973b-fa4072f0a39e
Newall, Tutte
dcb33a14-8cbb-4ab1-ade1-ad59d8a47efc
Griffiths, Helen
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Lotery, Andrew J.
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Ratnayaka, J. Arjuna
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Self, Jay E.
0f6efc58-ae24-4667-b8d6-6fafa849e389
Lee, Helena
5d36fd1e-9334-4db5-b201-034d147133fb

Sanchez-Bretano, Aida, Keeling, Eloise, Scott, Jennifer A., Lynn, Savannah A., Soundara-Pandi, Sudha Priya, Macdonald, Sarah L., Newall, Tutte, Griffiths, Helen, Lotery, Andrew J., Ratnayaka, J. Arjuna, Self, Jay E. and Lee, Helena (2023) Human equivalent doses of l-DOPA rescues retinal morphology and visual function in a murine model of albinism. Scientific Reports, 13, [17173]. (doi:10.1038/s41598-023-44373-3).

Record type: Article

Abstract

l-DOPA is deficient in the developing albino eye, resulting in abnormalities of retinal development and visual impairment. Ongoing retinal development after birth has also been demonstrated in the developing albino eye offering a potential therapeutic window in humans. To study whether human equivalent doses of l-DOPA/Carbidopa administered during the crucial postnatal period of neuroplasticity can rescue visual function, OCA C57BL/6 J-c2J OCA1 mice were treated with a 28-day course of oral l-DOPA/Carbidopa at 3 different doses from 15 to 43 days postnatal age (PNA) and for 3 different lengths of treatment, to identify optimum dosage and treatment length. Visual electrophysiology, acuity, and retinal morphology were measured at 4, 5, 6, 12 and 16 weeks PNA and compared to untreated C57BL/6 J (WT) and OCA1 mice. Quantification of PEDF, βIII-tubulin and syntaxin-3 expression was also performed. Our data showed impaired retinal morphology, decreased retinal function and lower visual acuity in untreated OCA1 mice compared to WT mice. These changes were diminished or eliminated when treated with higher doses of l-DOPA/Carbidopa. Our results demonstrate that oral l-DOPA/Carbidopa supplementation at human equivalent doses during the postnatal critical period of retinal neuroplasticity can rescue visual retinal morphology and retinal function, via PEDF upregulation and modulation of retinal synaptogenesis, providing a further step towards developing an effective treatment for albinism patients.

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s41598-023-44373-3 - Version of Record
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Accepted/In Press date: 7 October 2023
e-pub ahead of print date: 11 October 2023
Additional Information: Funding Information: The authors would like to acknowledge Dr. Neil Smyth for providing veterinary support and advice for this project. The authors gratefully acknowledge use of the services and facilities of the Biomedical Research Facility at the University of Southampton. Funding Information: This work was funded by awards to HL from the Medical Research Council (MRC), London, UK (grant number: MR/R007640/1) and the Gift of Sight charity.

Identifiers

Local EPrints ID: 483255
URI: http://eprints.soton.ac.uk/id/eprint/483255
ISSN: 2045-2322
PURE UUID: 405a34ad-752d-4dd2-8b89-53d381103ebe
ORCID for Eloise Keeling: ORCID iD orcid.org/0000-0003-0399-359X
ORCID for Savannah A. Lynn: ORCID iD orcid.org/0000-0003-2513-3144
ORCID for Andrew J. Lotery: ORCID iD orcid.org/0000-0001-5541-4305
ORCID for J. Arjuna Ratnayaka: ORCID iD orcid.org/0000-0002-1027-6938
ORCID for Jay E. Self: ORCID iD orcid.org/0000-0002-1030-9963
ORCID for Helena Lee: ORCID iD orcid.org/0000-0002-2573-9536

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Date deposited: 26 Oct 2023 17:05
Last modified: 18 Mar 2024 03:52

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Contributors

Author: Aida Sanchez-Bretano
Author: Eloise Keeling ORCID iD
Author: Jennifer A. Scott
Author: Savannah A. Lynn ORCID iD
Author: Sudha Priya Soundara-Pandi
Author: Sarah L. Macdonald
Author: Tutte Newall
Author: Helen Griffiths
Author: Jay E. Self ORCID iD
Author: Helena Lee ORCID iD

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