Conserved Roles of the Prion Protein Domains on Subcellular Localization and Cell-Cell Adhesion

Analyses of cultured cells and transgenic mice expressing prion protein (PrP) deletion mutants have revealed that some properties of PrP -such as its ability to misfold, aggregate and trigger neurotoxicity- are controlled by discrete molecular determinants within its protein domains. Although the co...

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Autores principales: Solis, Gonzalo P., Radon, Yvonne, Sempou, Emily, Jechow, Katharina, Stuermer, Claudia A. O., Málaga-Trillo, Edward
Formato: Online Artículo Texto
Lenguaje:English
Publicado: Public Library of Science 2013
Materias:
Research Article
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC3729945/
https://www.ncbi.nlm.nih.gov/pubmed/23936187
http://dx.doi.org/10.1371/journal.pone.0070327
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author Solis, Gonzalo P.
Radon, Yvonne
Sempou, Emily
Jechow, Katharina
Stuermer, Claudia A. O.
Málaga-Trillo, Edward
author_facet Solis, Gonzalo P.
Radon, Yvonne
Sempou, Emily
Jechow, Katharina
Stuermer, Claudia A. O.
Málaga-Trillo, Edward
author_sort Solis, Gonzalo P.
collection PubMed
description Analyses of cultured cells and transgenic mice expressing prion protein (PrP) deletion mutants have revealed that some properties of PrP -such as its ability to misfold, aggregate and trigger neurotoxicity- are controlled by discrete molecular determinants within its protein domains. Although the contributions of these determinants to PrP biosynthesis and turnover are relatively well characterized, it is still unclear how they modulate cellular functions of PrP. To address this question, we used two defined activities of PrP as functional readouts: 1) the recruitment of PrP to cell-cell contacts in Drosophila S2 and human MCF-7 epithelial cells, and 2) the induction of PrP embryonic loss- and gain-of-function phenotypes in zebrafish. Our results show that homologous mutations in mouse and zebrafish PrPs similarly affect their subcellular localization patterns as well as their in vitro and in vivo activities. Among PrP’s essential features, the N-terminal leader peptide was sufficient to drive targeting of our constructs to cell contact sites, whereas lack of GPI-anchoring and N-glycosylation rendered them inactive by blocking their cell surface expression. Importantly, our data suggest that the ability of PrP to homophilically trans-interact and elicit intracellular signaling is primarily encoded in its globular domain, and modulated by its repetitive domain. Thus, while the latter induces the local accumulation of PrPs at discrete punctae along cell contacts, the former counteracts this effect by promoting the continuous distribution of PrP. In early zebrafish embryos, deletion of either domain significantly impaired PrP’s ability to modulate E-cadherin cell adhesion. Altogether, these experiments relate structural features of PrP to its subcellular distribution and in vivo activity. Furthermore, they show that despite their large evolutionary history, the roles of PrP domains and posttranslational modifications are conserved between mouse and zebrafish.
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spelling pubmed-37299452013-08-09 Conserved Roles of the Prion Protein Domains on Subcellular Localization and Cell-Cell Adhesion Solis, Gonzalo P. Radon, Yvonne Sempou, Emily Jechow, Katharina Stuermer, Claudia A. O. Málaga-Trillo, Edward PLoS One Research Article Analyses of cultured cells and transgenic mice expressing prion protein (PrP) deletion mutants have revealed that some properties of PrP -such as its ability to misfold, aggregate and trigger neurotoxicity- are controlled by discrete molecular determinants within its protein domains. Although the contributions of these determinants to PrP biosynthesis and turnover are relatively well characterized, it is still unclear how they modulate cellular functions of PrP. To address this question, we used two defined activities of PrP as functional readouts: 1) the recruitment of PrP to cell-cell contacts in Drosophila S2 and human MCF-7 epithelial cells, and 2) the induction of PrP embryonic loss- and gain-of-function phenotypes in zebrafish. Our results show that homologous mutations in mouse and zebrafish PrPs similarly affect their subcellular localization patterns as well as their in vitro and in vivo activities. Among PrP’s essential features, the N-terminal leader peptide was sufficient to drive targeting of our constructs to cell contact sites, whereas lack of GPI-anchoring and N-glycosylation rendered them inactive by blocking their cell surface expression. Importantly, our data suggest that the ability of PrP to homophilically trans-interact and elicit intracellular signaling is primarily encoded in its globular domain, and modulated by its repetitive domain. Thus, while the latter induces the local accumulation of PrPs at discrete punctae along cell contacts, the former counteracts this effect by promoting the continuous distribution of PrP. In early zebrafish embryos, deletion of either domain significantly impaired PrP’s ability to modulate E-cadherin cell adhesion. Altogether, these experiments relate structural features of PrP to its subcellular distribution and in vivo activity. Furthermore, they show that despite their large evolutionary history, the roles of PrP domains and posttranslational modifications are conserved between mouse and zebrafish. Public Library of Science 2013-07-31 /pmc/articles/PMC3729945/ /pubmed/23936187 http://dx.doi.org/10.1371/journal.pone.0070327 Text en © 2013 Solis et al http://creativecommons.org/licenses/by/4.0/ This is an open-access article distributed under the terms of the Creative Commons Attribution License, which permits unrestricted use, distribution, and reproduction in any medium, provided the original author and source are properly credited.
spellingShingle Research Article
Solis, Gonzalo P.
Radon, Yvonne
Sempou, Emily
Jechow, Katharina
Stuermer, Claudia A. O.
Málaga-Trillo, Edward
Conserved Roles of the Prion Protein Domains on Subcellular Localization and Cell-Cell Adhesion
title Conserved Roles of the Prion Protein Domains on Subcellular Localization and Cell-Cell Adhesion
title_full Conserved Roles of the Prion Protein Domains on Subcellular Localization and Cell-Cell Adhesion
title_fullStr Conserved Roles of the Prion Protein Domains on Subcellular Localization and Cell-Cell Adhesion
title_full_unstemmed Conserved Roles of the Prion Protein Domains on Subcellular Localization and Cell-Cell Adhesion
title_short Conserved Roles of the Prion Protein Domains on Subcellular Localization and Cell-Cell Adhesion
title_sort conserved roles of the prion protein domains on subcellular localization and cell-cell adhesion
topic Research Article
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC3729945/
https://www.ncbi.nlm.nih.gov/pubmed/23936187
http://dx.doi.org/10.1371/journal.pone.0070327
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