Structural and mechanistic aspects influencing the ADAM10-mediated shedding of the prion protein

Structural and mechanistic aspects influencing the ADAM10-mediated shedding of the prion protein

Abstract Background Proteolytic processing of the prion protein (PrPC) by endogenous proteases generates bioactive membrane-bound and soluble fragments which may help to explain the pleiotropic roles of this protein in the nervous system and in brain diseases. Shedding of almost full-length PrPC int...

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Main Authors: Luise Linsenmeier, Behnam Mohammadi, Sebastian Wetzel, Berta Puig, Walker S. Jackson, Alexander Hartmann, Keiji Uchiyama, Suehiro Sakaguchi, Kristina Endres, Jörg Tatzelt, Paul Saftig, Markus Glatzel, Hermann C. Altmeppen
Format: Article
Language:English
Published: BMC 2018-04-01
Series:Molecular Neurodegeneration
Subjects:
ADAM10
Antibody
Exosomes
Glycosylation
Membrane anchor
Neurodegeneration
Online Access:http://link.springer.com/article/10.1186/s13024-018-0248-6
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spelling doaj-562e30b2afef436aa3c1b09eea5115722020-11-25T00:58:14ZengBMCMolecular Neurodegeneration1750-13262018-04-0113111710.1186/s13024-018-0248-6Structural and mechanistic aspects influencing the ADAM10-mediated shedding of the prion proteinLuise Linsenmeier0Behnam Mohammadi1Sebastian Wetzel2Berta Puig3Walker S. Jackson4Alexander Hartmann5Keiji Uchiyama6Suehiro Sakaguchi7Kristina Endres8Jörg Tatzelt9Paul Saftig10Markus Glatzel11Hermann C. Altmeppen12Institute of Neuropathology, University Medical Center Hamburg-Eppendorf (UKE)Institute of Neuropathology, University Medical Center Hamburg-Eppendorf (UKE)Institute of Biochemistry, Christian Albrechts UniversityInstitute of Neuropathology, University Medical Center Hamburg-Eppendorf (UKE)German Center for Neurodegenerative Diseases (DZNE)Institute of Neuropathology, University Medical Center Hamburg-Eppendorf (UKE)Division of Molecular Neurobiology, Institute of Enzyme Research, Tokushima UniversityDivision of Molecular Neurobiology, Institute of Enzyme Research, Tokushima UniversityDepartment of Psychiatry and Psychotherapy, University Medical Center, Johannes Gutenberg UniversityInstitute of Biochemistry and Pathobiochemistry, Ruhr UniversityInstitute of Biochemistry, Christian Albrechts UniversityInstitute of Neuropathology, University Medical Center Hamburg-Eppendorf (UKE)Institute of Neuropathology, University Medical Center Hamburg-Eppendorf (UKE)Abstract Background Proteolytic processing of the prion protein (PrPC) by endogenous proteases generates bioactive membrane-bound and soluble fragments which may help to explain the pleiotropic roles of this protein in the nervous system and in brain diseases. Shedding of almost full-length PrPC into the extracellular space by the metalloprotease ADAM10 is of peculiar relevance since soluble PrP stimulates axonal outgrowth and is protective in neurodegenerative conditions such as Alzheimer’s and prion disease. However, molecular determinates and mechanisms regulating the shedding of PrP are entirely unknown. Methods We produced an antibody recognizing the neo-epitope of shed PrP generated by ADAM10 in biological samples and used it to study structural and mechanistic aspects affecting the shedding. For this, we investigated genetically modified cellular and murine models by biochemical and morphological approaches. Results We show that the novel antibody specifically detects shed PrP in cell culture supernatants and murine brain. We demonstrate that ADAM10 is the exclusive sheddase of PrPC in the nervous system and reveal that the glycosylation state and type of membrane-anchorage of PrPC severely affect its shedding. Furthermore, we provide evidence that PrP shedding can be modulated by pharmacological inhibition and stimulation and present data suggesting that shedding is a relevant part of a compensatory network ensuring PrPC homeostasis of the cell. Conclusions With the new antibody, our study introduces a new tool to reliably investigate PrP-shedding. In addition, this study provides novel and important insight into the regulation of this cleavage event, which is likely to be relevant for diagnostic and therapeutic approaches even beyond neurodegeneration.http://link.springer.com/article/10.1186/s13024-018-0248-6ADAM10AntibodyExosomesGlycosylationMembrane anchorNeurodegeneration
collection DOAJ
language English
format Article
sources DOAJ
author Luise Linsenmeier
Behnam Mohammadi
Sebastian Wetzel
Berta Puig
Walker S. Jackson
Alexander Hartmann
Keiji Uchiyama
Suehiro Sakaguchi
Kristina Endres
Jörg Tatzelt
Paul Saftig
Markus Glatzel
Hermann C. Altmeppen
spellingShingle Luise Linsenmeier
Behnam Mohammadi
Sebastian Wetzel
Berta Puig
Walker S. Jackson
Alexander Hartmann
Keiji Uchiyama
Suehiro Sakaguchi
Kristina Endres
Jörg Tatzelt
Paul Saftig
Markus Glatzel
Hermann C. Altmeppen
Structural and mechanistic aspects influencing the ADAM10-mediated shedding of the prion protein
Molecular Neurodegeneration
ADAM10
Antibody
Exosomes
Glycosylation
Membrane anchor
Neurodegeneration
author_facet Luise Linsenmeier
Behnam Mohammadi
Sebastian Wetzel
Berta Puig
Walker S. Jackson
Alexander Hartmann
Keiji Uchiyama
Suehiro Sakaguchi
Kristina Endres
Jörg Tatzelt
Paul Saftig
Markus Glatzel
Hermann C. Altmeppen
author_sort Luise Linsenmeier
title Structural and mechanistic aspects influencing the ADAM10-mediated shedding of the prion protein
title_short Structural and mechanistic aspects influencing the ADAM10-mediated shedding of the prion protein
title_full Structural and mechanistic aspects influencing the ADAM10-mediated shedding of the prion protein
title_fullStr Structural and mechanistic aspects influencing the ADAM10-mediated shedding of the prion protein
title_full_unstemmed Structural and mechanistic aspects influencing the ADAM10-mediated shedding of the prion protein
title_sort structural and mechanistic aspects influencing the adam10-mediated shedding of the prion protein
publisher BMC
series Molecular Neurodegeneration
issn 1750-1326
publishDate 2018-04-01
description Abstract Background Proteolytic processing of the prion protein (PrPC) by endogenous proteases generates bioactive membrane-bound and soluble fragments which may help to explain the pleiotropic roles of this protein in the nervous system and in brain diseases. Shedding of almost full-length PrPC into the extracellular space by the metalloprotease ADAM10 is of peculiar relevance since soluble PrP stimulates axonal outgrowth and is protective in neurodegenerative conditions such as Alzheimer’s and prion disease. However, molecular determinates and mechanisms regulating the shedding of PrP are entirely unknown. Methods We produced an antibody recognizing the neo-epitope of shed PrP generated by ADAM10 in biological samples and used it to study structural and mechanistic aspects affecting the shedding. For this, we investigated genetically modified cellular and murine models by biochemical and morphological approaches. Results We show that the novel antibody specifically detects shed PrP in cell culture supernatants and murine brain. We demonstrate that ADAM10 is the exclusive sheddase of PrPC in the nervous system and reveal that the glycosylation state and type of membrane-anchorage of PrPC severely affect its shedding. Furthermore, we provide evidence that PrP shedding can be modulated by pharmacological inhibition and stimulation and present data suggesting that shedding is a relevant part of a compensatory network ensuring PrPC homeostasis of the cell. Conclusions With the new antibody, our study introduces a new tool to reliably investigate PrP-shedding. In addition, this study provides novel and important insight into the regulation of this cleavage event, which is likely to be relevant for diagnostic and therapeutic approaches even beyond neurodegeneration.
topic ADAM10
Antibody
Exosomes
Glycosylation
Membrane anchor
Neurodegeneration
url http://link.springer.com/article/10.1186/s13024-018-0248-6
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