Therapeutic potential of archaeal unfoldase PAN.sup.et and the gateless T20S proteasome in P23H rhodopsin retinitis pigmentosa mice

Therapeutic potential of archaeal unfoldase PAN.sup.et and the gateless T20S proteasome in P23H rhodopsin retinitis pigmentosa mice

Neurodegenerative diseases are characterized by the presence of misfolded and aggregated proteins which are thought to contribute to the development of the disease. In one form of inherited blinding disease, retinitis pigmentosa, a P23H mutation in the light-sensing receptor, rhodopsin causes rhodop...

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Veröffentlicht in:PloS one 2024-10, Vol.19 (10), p.e0308058
Hauptverfasser: Brooks, Celine, Kolson, Douglas, Sechrest, Emily, Chuah, Janelle, Schupp, Jane, Billington, Neil, Deng, Wen-Tao, Smith, David, Sokolov, Maxim
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Care and treatment
Diagnosis
Genetic aspects
Health aspects
Nervous system diseases
Proteins
Proteolysis
Retinitis pigmentosa
Rhodopsin
Scientific equipment and supplies industry
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container_issue 10
container_start_page e0308058
container_title PloS one
container_volume 19
creator Brooks, Celine
Kolson, Douglas
Sechrest, Emily
Chuah, Janelle
Schupp, Jane
Billington, Neil
Deng, Wen-Tao
Smith, David
Sokolov, Maxim
description Neurodegenerative diseases are characterized by the presence of misfolded and aggregated proteins which are thought to contribute to the development of the disease. In one form of inherited blinding disease, retinitis pigmentosa, a P23H mutation in the light-sensing receptor, rhodopsin causes rhodopsin misfolding resulting in complete vision loss. We investigated whether a xenogeneic protein-unfolding ATPase (unfoldase) from thermophilic Archaea, termed PAN.sup.et, could counteract the proteotoxicity of P23H rhodopsin. We found that PAN.sup.et increased the number of surviving photoreceptors in P23H rhodopsin mice and recognized rhodopsin as a substate in vitro. This data supports the feasibility and efficacy of using a xenogeneic unfoldase as a therapeutic approach in mouse models of human neurodegenerative diseases. We also showed that an archaeal proteasome, called the T20S can degrade rhodopsin in vitro and demonstrated that it is feasible and safe to express gateless T20S proteasomes in vivo in mouse rod photoreceptors. Expression of archaeal proteasomes may be an effective therapeutic approach to stimulate protein degradation in retinopathies and neurodegenerative diseases with protein-misfolding etiology.
doi_str_mv 10.1371/journal.pone.0308058
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subjects Care and treatment
Diagnosis
Genetic aspects
Health aspects
Nervous system diseases
Proteins
Proteolysis
Retinitis pigmentosa
Rhodopsin
Scientific equipment and supplies industry
title Therapeutic potential of archaeal unfoldase PAN.sup.et and the gateless T20S proteasome in P23H rhodopsin retinitis pigmentosa mice
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