Membrane-enriched proteome changes and prion protein expression during neural differentiation and in neuroblastoma cells

Membrane-enriched proteome changes and prion protein expression during neural differentiation and in neuroblastoma cells

Abstract Background The function of the prion protein, involved in the so-called prion diseases, remains a subject of intense debate and the possibility that it works as a pleiotropic protein through the interaction with multiple membrane proteins is somehow supported by recent reports. Therefore, t...

Full description

Bibliographic Details
Main Authors: J. A. Macedo, D. Schrama, I. Duarte, E. Tavares, J. Renaut, M. E. Futschik, P. M. Rodrigues, E. P. Melo
Format: Article
Language:English
Published: BMC 2017-04-01
Series:BMC Genomics
Subjects:
Prion protein
2D-DIGE
Neural differentiation
Chaperone activity
Redox homeostasis
Online Access:http://link.springer.com/article/10.1186/s12864-017-3694-6
id doaj-a4aa0f5dd20f40789bba93673e431fed
record_format Article
spelling doaj-a4aa0f5dd20f40789bba93673e431fed2020-11-25T01:07:27ZengBMCBMC Genomics1471-21642017-04-0118111310.1186/s12864-017-3694-6Membrane-enriched proteome changes and prion protein expression during neural differentiation and in neuroblastoma cellsJ. A. Macedo0D. Schrama1I. Duarte2E. Tavares3J. Renaut4M. E. Futschik5P. M. Rodrigues6E. P. Melo7CBMR, Center for Biomedical Research, University of AlgarveCCMAR, Centre of Marine Sciences of Algarve, University of AlgarveCBMR, Center for Biomedical Research, University of AlgarveCBMR, Center for Biomedical Research, University of AlgarveLIST, Luxembourg Institute of Science and TechnologyCCMAR, Centre of Marine Sciences of Algarve, University of AlgarveCCMAR, Centre of Marine Sciences of Algarve, University of AlgarveCBMR, Center for Biomedical Research, University of AlgarveAbstract Background The function of the prion protein, involved in the so-called prion diseases, remains a subject of intense debate and the possibility that it works as a pleiotropic protein through the interaction with multiple membrane proteins is somehow supported by recent reports. Therefore, the use of proteomic and bioinformatics combined to uncover cellular processes occurring together with changes in the expression of the prion protein may provide further insight into the putative pleiotropic role of the prion protein. Results This study assessed the membrane-enriched proteome changes accompanying alterations in the expression of the prion protein. A 2D-DIGE approach was applied to two cell lines after prefractionation towards the membrane protein subset: an embryonic stem cell line and the PK1 subline of neuroblastoma cells which efficiently propagates prion infection. Several proteins were differentially abundant with the increased expression of the prion protein during neural differentiation of embryonic stem cells and with the knockdown of the prion protein in PK1 cells. The identity of around 20% of the differentially abundant proteins was obtained by tandem MS. The catalytic subunit A of succinate dehydrogenase, a key enzyme for the aerobic energy metabolism and redox homeostasis, showed a similar abundance trend as the prion protein in both proteomic experiments. A gene ontology analysis revealed “myelin sheath”, “organelle membrane” and “focal adhesion” associated proteins as the main cellular components, and “protein folding” and “ATPase activity” as the biological processes enriched in the first set of differentially abundant proteins. The known interactome of these differentially abundant proteins was customized to reveal four interactors with the prion protein, including two heat shock proteins and a protein disulfide isomerase. Conclusions Overall, our study shows that expression of the prion protein occurs concomitantly with changes in chaperone activity and cell-redox homeostasis, emphasizing the functional link between these cellular processes and the prion protein.http://link.springer.com/article/10.1186/s12864-017-3694-6Prion protein2D-DIGENeural differentiationChaperone activityRedox homeostasis
collection DOAJ
language English
format Article
sources DOAJ
author J. A. Macedo
D. Schrama
I. Duarte
E. Tavares
J. Renaut
M. E. Futschik
P. M. Rodrigues
E. P. Melo
spellingShingle J. A. Macedo
D. Schrama
I. Duarte
E. Tavares
J. Renaut
M. E. Futschik
P. M. Rodrigues
E. P. Melo
Membrane-enriched proteome changes and prion protein expression during neural differentiation and in neuroblastoma cells
BMC Genomics
Prion protein
2D-DIGE
Neural differentiation
Chaperone activity
Redox homeostasis
author_facet J. A. Macedo
D. Schrama
I. Duarte
E. Tavares
J. Renaut
M. E. Futschik
P. M. Rodrigues
E. P. Melo
author_sort J. A. Macedo
title Membrane-enriched proteome changes and prion protein expression during neural differentiation and in neuroblastoma cells
title_short Membrane-enriched proteome changes and prion protein expression during neural differentiation and in neuroblastoma cells
title_full Membrane-enriched proteome changes and prion protein expression during neural differentiation and in neuroblastoma cells
title_fullStr Membrane-enriched proteome changes and prion protein expression during neural differentiation and in neuroblastoma cells
title_full_unstemmed Membrane-enriched proteome changes and prion protein expression during neural differentiation and in neuroblastoma cells
title_sort membrane-enriched proteome changes and prion protein expression during neural differentiation and in neuroblastoma cells
publisher BMC
series BMC Genomics
issn 1471-2164
publishDate 2017-04-01
description Abstract Background The function of the prion protein, involved in the so-called prion diseases, remains a subject of intense debate and the possibility that it works as a pleiotropic protein through the interaction with multiple membrane proteins is somehow supported by recent reports. Therefore, the use of proteomic and bioinformatics combined to uncover cellular processes occurring together with changes in the expression of the prion protein may provide further insight into the putative pleiotropic role of the prion protein. Results This study assessed the membrane-enriched proteome changes accompanying alterations in the expression of the prion protein. A 2D-DIGE approach was applied to two cell lines after prefractionation towards the membrane protein subset: an embryonic stem cell line and the PK1 subline of neuroblastoma cells which efficiently propagates prion infection. Several proteins were differentially abundant with the increased expression of the prion protein during neural differentiation of embryonic stem cells and with the knockdown of the prion protein in PK1 cells. The identity of around 20% of the differentially abundant proteins was obtained by tandem MS. The catalytic subunit A of succinate dehydrogenase, a key enzyme for the aerobic energy metabolism and redox homeostasis, showed a similar abundance trend as the prion protein in both proteomic experiments. A gene ontology analysis revealed “myelin sheath”, “organelle membrane” and “focal adhesion” associated proteins as the main cellular components, and “protein folding” and “ATPase activity” as the biological processes enriched in the first set of differentially abundant proteins. The known interactome of these differentially abundant proteins was customized to reveal four interactors with the prion protein, including two heat shock proteins and a protein disulfide isomerase. Conclusions Overall, our study shows that expression of the prion protein occurs concomitantly with changes in chaperone activity and cell-redox homeostasis, emphasizing the functional link between these cellular processes and the prion protein.
topic Prion protein
2D-DIGE
Neural differentiation
Chaperone activity
Redox homeostasis
url http://link.springer.com/article/10.1186/s12864-017-3694-6
work_keys_str_mv AT jamacedo membraneenrichedproteomechangesandprionproteinexpressionduringneuraldifferentiationandinneuroblastomacells
AT dschrama membraneenrichedproteomechangesandprionproteinexpressionduringneuraldifferentiationandinneuroblastomacells
AT iduarte membraneenrichedproteomechangesandprionproteinexpressionduringneuraldifferentiationandinneuroblastomacells
AT etavares membraneenrichedproteomechangesandprionproteinexpressionduringneuraldifferentiationandinneuroblastomacells
AT jrenaut membraneenrichedproteomechangesandprionproteinexpressionduringneuraldifferentiationandinneuroblastomacells
AT mefutschik membraneenrichedproteomechangesandprionproteinexpressionduringneuraldifferentiationandinneuroblastomacells
AT pmrodrigues membraneenrichedproteomechangesandprionproteinexpressionduringneuraldifferentiationandinneuroblastomacells
AT epmelo membraneenrichedproteomechangesandprionproteinexpressionduringneuraldifferentiationandinneuroblastomacells
_version_ 1725187194495172608

Similar Items