Cardiac glycoside-mediated turnover of Na, K-ATPases as a rational approach to reducing cell surface levels of the cellular prion protein

It is widely anticipated that a reduction of brain levels of the cellular prion protein (PrP(C)) can prolong survival in a group of neurodegenerative diseases known as prion diseases. To date, efforts to decrease steady-state PrP(C) levels by targeting this protein directly with small molecule drug-...

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Autores principales: Mehrabian, Mohadeseh, Wang, Xinzhu, Eid, Shehab, Yan, Bei Qi, Grinberg, Mark, Siegner, Murdock, Sackmann, Christopher, Sulman, Muhammad, Zhao, Wenda, Williams, Declan, Schmitt-Ulms, Gerold
Formato: Online Artículo Texto
Lenguaje:English
Publicado: Public Library of Science 2022
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Research Article
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC9249225/
https://www.ncbi.nlm.nih.gov/pubmed/35776750
http://dx.doi.org/10.1371/journal.pone.0270915
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author Mehrabian, Mohadeseh
Wang, Xinzhu
Eid, Shehab
Yan, Bei Qi
Grinberg, Mark
Siegner, Murdock
Sackmann, Christopher
Sulman, Muhammad
Zhao, Wenda
Williams, Declan
Schmitt-Ulms, Gerold
author_facet Mehrabian, Mohadeseh
Wang, Xinzhu
Eid, Shehab
Yan, Bei Qi
Grinberg, Mark
Siegner, Murdock
Sackmann, Christopher
Sulman, Muhammad
Zhao, Wenda
Williams, Declan
Schmitt-Ulms, Gerold
author_sort Mehrabian, Mohadeseh
collection PubMed
description It is widely anticipated that a reduction of brain levels of the cellular prion protein (PrP(C)) can prolong survival in a group of neurodegenerative diseases known as prion diseases. To date, efforts to decrease steady-state PrP(C) levels by targeting this protein directly with small molecule drug-like compounds have largely been unsuccessful. Recently, we reported Na,K-ATPases to reside in immediate proximity to PrP(C) in the brain, unlocking an opportunity for an indirect PrP(C) targeting approach that capitalizes on the availability of potent cardiac glycosides (CGs). Here, we report that exposure of human co-cultures of neurons and astrocytes to non-toxic nanomolar levels of CGs causes profound reductions in PrP(C) levels. The mechanism of action underpinning this outcome relies primarily on a subset of CGs engaging the ATP1A1 isoform, one of three α subunits of Na,K-ATPases expressed in brain cells. Upon CG docking to ATP1A1, the ligand receptor complex, and PrP(C) along with it, is internalized by the cell. Subsequently, PrP(C) is channeled to the lysosomal compartment where it is digested in a manner that can be rescued by silencing the cysteine protease cathepsin B. These data signify that the repurposing of CGs may be beneficial for the treatment of prion disorders.
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spelling pubmed-92492252022-07-02 Cardiac glycoside-mediated turnover of Na, K-ATPases as a rational approach to reducing cell surface levels of the cellular prion protein Mehrabian, Mohadeseh Wang, Xinzhu Eid, Shehab Yan, Bei Qi Grinberg, Mark Siegner, Murdock Sackmann, Christopher Sulman, Muhammad Zhao, Wenda Williams, Declan Schmitt-Ulms, Gerold PLoS One Research Article It is widely anticipated that a reduction of brain levels of the cellular prion protein (PrP(C)) can prolong survival in a group of neurodegenerative diseases known as prion diseases. To date, efforts to decrease steady-state PrP(C) levels by targeting this protein directly with small molecule drug-like compounds have largely been unsuccessful. Recently, we reported Na,K-ATPases to reside in immediate proximity to PrP(C) in the brain, unlocking an opportunity for an indirect PrP(C) targeting approach that capitalizes on the availability of potent cardiac glycosides (CGs). Here, we report that exposure of human co-cultures of neurons and astrocytes to non-toxic nanomolar levels of CGs causes profound reductions in PrP(C) levels. The mechanism of action underpinning this outcome relies primarily on a subset of CGs engaging the ATP1A1 isoform, one of three α subunits of Na,K-ATPases expressed in brain cells. Upon CG docking to ATP1A1, the ligand receptor complex, and PrP(C) along with it, is internalized by the cell. Subsequently, PrP(C) is channeled to the lysosomal compartment where it is digested in a manner that can be rescued by silencing the cysteine protease cathepsin B. These data signify that the repurposing of CGs may be beneficial for the treatment of prion disorders. Public Library of Science 2022-07-01 /pmc/articles/PMC9249225/ /pubmed/35776750 http://dx.doi.org/10.1371/journal.pone.0270915 Text en © 2022 Mehrabian et al https://creativecommons.org/licenses/by/4.0/This is an open access article distributed under the terms of the Creative Commons Attribution License (https://creativecommons.org/licenses/by/4.0/) , which permits unrestricted use, distribution, and reproduction in any medium, provided the original author and source are credited.
spellingShingle Research Article
Mehrabian, Mohadeseh
Wang, Xinzhu
Eid, Shehab
Yan, Bei Qi
Grinberg, Mark
Siegner, Murdock
Sackmann, Christopher
Sulman, Muhammad
Zhao, Wenda
Williams, Declan
Schmitt-Ulms, Gerold
Cardiac glycoside-mediated turnover of Na, K-ATPases as a rational approach to reducing cell surface levels of the cellular prion protein
title Cardiac glycoside-mediated turnover of Na, K-ATPases as a rational approach to reducing cell surface levels of the cellular prion protein
title_full Cardiac glycoside-mediated turnover of Na, K-ATPases as a rational approach to reducing cell surface levels of the cellular prion protein
title_fullStr Cardiac glycoside-mediated turnover of Na, K-ATPases as a rational approach to reducing cell surface levels of the cellular prion protein
title_full_unstemmed Cardiac glycoside-mediated turnover of Na, K-ATPases as a rational approach to reducing cell surface levels of the cellular prion protein
title_short Cardiac glycoside-mediated turnover of Na, K-ATPases as a rational approach to reducing cell surface levels of the cellular prion protein
title_sort cardiac glycoside-mediated turnover of na, k-atpases as a rational approach to reducing cell surface levels of the cellular prion protein
topic Research Article
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC9249225/
https://www.ncbi.nlm.nih.gov/pubmed/35776750
http://dx.doi.org/10.1371/journal.pone.0270915
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