Multiple system atrophy-associated oligodendroglial protein p25α stimulates formation of novel α-synuclein strain with enhanced neurodegenerative potential

Nelson Ferreira; Hjalte Gram; Zachary A. Sorrentino; Emil Gregersen; Sissel Ida Schmidt; Lasse Reimer; Cristine Betzer; Clara Perez-Gozalbo; Marjo Beltoja; Madhu Nagaraj; Jie Wang; Jan S. Nowak; Mingdong Dong; Katarina Willén; Ersoy Cholak; Kaare Bjerregaard-Andersen; Nicolas Mendez; Prakruti Rabadia; Mohammad Shahnawaz; Claudio Soto; Daniel E. Otzen; Ümit Akbey; Morten Meyer; Benoit I. Giasson; Marina Romero-Ramos; Poul Henning Jensen

doi:10.1007/s00401-021-02316-0

Multiple system atrophy-associated oligodendroglial protein p25α stimulates formation of novel α-synuclein strain with enhanced neurodegenerative potential

Nelson Ferreira^*, Hjalte Gram, Zachary A. Sorrentino, Emil Gregersen, Sissel Ida Schmidt, Lasse Reimer, Cristine Betzer, Clara Perez-Gozalbo, Marjo Beltoja, Madhu Nagaraj, Jie Wang, Jan S. Nowak, Mingdong Dong, Katarina Willén, Ersoy Cholak, Kaare Bjerregaard-Andersen, Nicolas Mendez, Prakruti Rabadia, Mohammad Shahnawaz, Claudio SotoDaniel E. Otzen, Ümit Akbey, Morten Meyer, Benoit I. Giasson, Marina Romero-Ramos, Poul Henning Jensen

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Abstract

Pathology consisting of intracellular aggregates of alpha-Synuclein (α-Syn) spread through the nervous system in a variety of neurodegenerative disorders including Parkinson’s disease, dementia with Lewy bodies, and multiple system atrophy. The discovery of structurally distinct α-Syn polymorphs, so-called strains, supports a hypothesis where strain-specific structures are templated into aggregates formed by native α-Syn. These distinct strains are hypothesised to dictate the spreading of pathology in the tissue and the cellular impact of the aggregates, thereby contributing to the variety of clinical phenotypes. Here, we present evidence of a novel α-Syn strain induced by the multiple system atrophy-associated oligodendroglial protein p25α. Using an array of biophysical, biochemical, cellular, and in vivo analyses, we demonstrate that compared to α-Syn alone, a substoichiometric concentration of p25α redirects α-Syn aggregation into a unique α-Syn/p25α strain with a different structure and enhanced in vivo prodegenerative properties. The α-Syn/p25α strain induced larger inclusions in human dopaminergic neurons. In vivo, intramuscular injection of preformed fibrils (PFF) of the α-Syn/p25α strain compared to α-Syn PFF resulted in a shortened life span and a distinct anatomical distribution of inclusion pathology in the brain of a human A53T transgenic (line M83) mouse. Investigation of α-Syn aggregates in brain stem extracts of end-stage mice demonstrated that the more aggressive phenotype of the α-Syn/p25α strain was associated with an increased load of α-Syn aggregates based on a Förster resonance energy transfer immunoassay and a reduced α-Syn aggregate seeding activity based on a protein misfolding cyclic amplification assay. When injected unilaterally into the striata of wild-type mice, the α-Syn/p25α strain resulted in a more-pronounced motoric phenotype than α-Syn PFF and exhibited a “tropism” for nigro-striatal neurons compared to α-Syn PFF. Overall, our data support a hypothesis whereby oligodendroglial p25α is responsible for generating a highly prodegenerative α-Syn strain in multiple system atrophy.

Originalsprog	Engelsk
Tidsskrift	Acta Neuropathologica
Vol/bind	142
Udgave nummer	1
Sider (fra-til)	87-115
ISSN	0001-6322
DOI	https://doi.org/10.1007/s00401-021-02316-0
Status	Udgivet - jul. 2021

Bibliografisk note

Funding Information:
The study was supported by Lundbeck Foundation grants R223-2015-4222 for PHJ, R248-2016-2518 for Danish Research Institute of Translational Neuroscience-DANDRITE, Nordic-EMBL Partnership for Molecular Medicine, Aarhus University, Denmark, Postdoctoral Fellowship R171-2014-591 to N.F. and R276-2018-671 to D.E.O and J.S.N. The National Institutes of Health R01NS100876 to B.I.G., Danish Council for Independent Research Grant ID: 6108-00396B to M.D., a Predoctoral Fellowship F30AG063446 to Z.A.S. This work was funded in part by a grant from the Michael J Fox Foundation for Parkinson’s Research to C.S. The authors would like to thank Marie Vestergaard for graphical data analysis with R programming and Jette Bank Lauridsen and Gitte Ulberg Toft for excellent technical assistance.

Publisher Copyright:
© 2021, The Author(s).

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10.1007/s00401-021-02316-0Licens: CC BY

Open Access VersionForlagets udgivne version, 11,9 MBLicens: CC BY

Citationsformater

Ferreira, N., Gram, H., Sorrentino, Z. A., Gregersen, E., Schmidt, S. I., Reimer, L., Betzer, C., Perez-Gozalbo, C., Beltoja, M., Nagaraj, M., Wang, J., Nowak, J. S., Dong, M., Willén, K., Cholak, E., Bjerregaard-Andersen, K., Mendez, N., Rabadia, P., Shahnawaz, M., ... Jensen, P. H. (2021). Multiple system atrophy-associated oligodendroglial protein p25α stimulates formation of novel α-synuclein strain with enhanced neurodegenerative potential. Acta Neuropathologica, 142(1), 87-115. https://doi.org/10.1007/s00401-021-02316-0

@article{d461774db096452a8f8be0a3e3084137,

title = "Multiple system atrophy-associated oligodendroglial protein p25α stimulates formation of novel α-synuclein strain with enhanced neurodegenerative potential",

abstract = "Pathology consisting of intracellular aggregates of alpha-Synuclein (α-Syn) spread through the nervous system in a variety of neurodegenerative disorders including Parkinson{\textquoteright}s disease, dementia with Lewy bodies, and multiple system atrophy. The discovery of structurally distinct α-Syn polymorphs, so-called strains, supports a hypothesis where strain-specific structures are templated into aggregates formed by native α-Syn. These distinct strains are hypothesised to dictate the spreading of pathology in the tissue and the cellular impact of the aggregates, thereby contributing to the variety of clinical phenotypes. Here, we present evidence of a novel α-Syn strain induced by the multiple system atrophy-associated oligodendroglial protein p25α. Using an array of biophysical, biochemical, cellular, and in vivo analyses, we demonstrate that compared to α-Syn alone, a substoichiometric concentration of p25α redirects α-Syn aggregation into a unique α-Syn/p25α strain with a different structure and enhanced in vivo prodegenerative properties. The α-Syn/p25α strain induced larger inclusions in human dopaminergic neurons. In vivo, intramuscular injection of preformed fibrils (PFF) of the α-Syn/p25α strain compared to α-Syn PFF resulted in a shortened life span and a distinct anatomical distribution of inclusion pathology in the brain of a human A53T transgenic (line M83) mouse. Investigation of α-Syn aggregates in brain stem extracts of end-stage mice demonstrated that the more aggressive phenotype of the α-Syn/p25α strain was associated with an increased load of α-Syn aggregates based on a F{\"o}rster resonance energy transfer immunoassay and a reduced α-Syn aggregate seeding activity based on a protein misfolding cyclic amplification assay. When injected unilaterally into the striata of wild-type mice, the α-Syn/p25α strain resulted in a more-pronounced motoric phenotype than α-Syn PFF and exhibited a “tropism” for nigro-striatal neurons compared to α-Syn PFF. Overall, our data support a hypothesis whereby oligodendroglial p25α is responsible for generating a highly prodegenerative α-Syn strain in multiple system atrophy.",

keywords = "Multiple system atrophy (MSA), P25α, Protein aggregation, Strains, Tubulin polymerisation-promoting protein (TPPP), Α-Synuclein",

author = "Nelson Ferreira and Hjalte Gram and Sorrentino, {Zachary A.} and Emil Gregersen and Schmidt, {Sissel Ida} and Lasse Reimer and Cristine Betzer and Clara Perez-Gozalbo and Marjo Beltoja and Madhu Nagaraj and Jie Wang and Nowak, {Jan S.} and Mingdong Dong and Katarina Will{\'e}n and Ersoy Cholak and Kaare Bjerregaard-Andersen and Nicolas Mendez and Prakruti Rabadia and Mohammad Shahnawaz and Claudio Soto and Otzen, {Daniel E.} and {\"U}mit Akbey and Morten Meyer and Giasson, {Benoit I.} and Marina Romero-Ramos and Jensen, {Poul Henning}",

note = "Funding Information: The study was supported by Lundbeck Foundation grants R223-2015-4222 for PHJ, R248-2016-2518 for Danish Research Institute of Translational Neuroscience-DANDRITE, Nordic-EMBL Partnership for Molecular Medicine, Aarhus University, Denmark, Postdoctoral Fellowship R171-2014-591 to N.F. and R276-2018-671 to D.E.O and J.S.N. The National Institutes of Health R01NS100876 to B.I.G., Danish Council for Independent Research Grant ID: 6108-00396B to M.D., a Predoctoral Fellowship F30AG063446 to Z.A.S. This work was funded in part by a grant from the Michael J Fox Foundation for Parkinson{\textquoteright}s Research to C.S. The authors would like to thank Marie Vestergaard for graphical data analysis with R programming and Jette Bank Lauridsen and Gitte Ulberg Toft for excellent technical assistance. Publisher Copyright: {\textcopyright} 2021, The Author(s).",

year = "2021",

month = jul,

doi = "10.1007/s00401-021-02316-0",

language = "English",

volume = "142",

pages = "87--115",

journal = "Acta Neuropathologica",

issn = "0001-6322",

publisher = "Springer",

number = "1",

}

Ferreira, N, Gram, H, Sorrentino, ZA, Gregersen, E, Schmidt, SI, Reimer, L, Betzer, C, Perez-Gozalbo, C, Beltoja, M, Nagaraj, M, Wang, J, Nowak, JS, Dong, M, Willén, K, Cholak, E, Bjerregaard-Andersen, K, Mendez, N, Rabadia, P, Shahnawaz, M, Soto, C, Otzen, DE, Akbey, Ü, Meyer, M, Giasson, BI, Romero-Ramos, M & Jensen, PH 2021, 'Multiple system atrophy-associated oligodendroglial protein p25α stimulates formation of novel α-synuclein strain with enhanced neurodegenerative potential', Acta Neuropathologica, bind 142, nr. 1, s. 87-115. https://doi.org/10.1007/s00401-021-02316-0

Multiple system atrophy-associated oligodendroglial protein p25α stimulates formation of novel α-synuclein strain with enhanced neurodegenerative potential. / Ferreira, Nelson; Gram, Hjalte; Sorrentino, Zachary A. et al.
I: Acta Neuropathologica, Bind 142, Nr. 1, 07.2021, s. 87-115.

Publikation: Bidrag til tidsskrift › Tidsskriftartikel › Forskning › peer review

TY - JOUR

T1 - Multiple system atrophy-associated oligodendroglial protein p25α stimulates formation of novel α-synuclein strain with enhanced neurodegenerative potential

AU - Ferreira, Nelson

AU - Gram, Hjalte

AU - Sorrentino, Zachary A.

AU - Gregersen, Emil

AU - Schmidt, Sissel Ida

AU - Reimer, Lasse

AU - Betzer, Cristine

AU - Perez-Gozalbo, Clara

AU - Beltoja, Marjo

AU - Nagaraj, Madhu

AU - Wang, Jie

AU - Nowak, Jan S.

AU - Dong, Mingdong

AU - Willén, Katarina

AU - Cholak, Ersoy

AU - Bjerregaard-Andersen, Kaare

AU - Mendez, Nicolas

AU - Rabadia, Prakruti

AU - Shahnawaz, Mohammad

AU - Soto, Claudio

AU - Otzen, Daniel E.

AU - Akbey, Ümit

AU - Meyer, Morten

AU - Giasson, Benoit I.

AU - Romero-Ramos, Marina

AU - Jensen, Poul Henning

N1 - Funding Information: The study was supported by Lundbeck Foundation grants R223-2015-4222 for PHJ, R248-2016-2518 for Danish Research Institute of Translational Neuroscience-DANDRITE, Nordic-EMBL Partnership for Molecular Medicine, Aarhus University, Denmark, Postdoctoral Fellowship R171-2014-591 to N.F. and R276-2018-671 to D.E.O and J.S.N. The National Institutes of Health R01NS100876 to B.I.G., Danish Council for Independent Research Grant ID: 6108-00396B to M.D., a Predoctoral Fellowship F30AG063446 to Z.A.S. This work was funded in part by a grant from the Michael J Fox Foundation for Parkinson’s Research to C.S. The authors would like to thank Marie Vestergaard for graphical data analysis with R programming and Jette Bank Lauridsen and Gitte Ulberg Toft for excellent technical assistance. Publisher Copyright: © 2021, The Author(s).

PY - 2021/7

Y1 - 2021/7

N2 - Pathology consisting of intracellular aggregates of alpha-Synuclein (α-Syn) spread through the nervous system in a variety of neurodegenerative disorders including Parkinson’s disease, dementia with Lewy bodies, and multiple system atrophy. The discovery of structurally distinct α-Syn polymorphs, so-called strains, supports a hypothesis where strain-specific structures are templated into aggregates formed by native α-Syn. These distinct strains are hypothesised to dictate the spreading of pathology in the tissue and the cellular impact of the aggregates, thereby contributing to the variety of clinical phenotypes. Here, we present evidence of a novel α-Syn strain induced by the multiple system atrophy-associated oligodendroglial protein p25α. Using an array of biophysical, biochemical, cellular, and in vivo analyses, we demonstrate that compared to α-Syn alone, a substoichiometric concentration of p25α redirects α-Syn aggregation into a unique α-Syn/p25α strain with a different structure and enhanced in vivo prodegenerative properties. The α-Syn/p25α strain induced larger inclusions in human dopaminergic neurons. In vivo, intramuscular injection of preformed fibrils (PFF) of the α-Syn/p25α strain compared to α-Syn PFF resulted in a shortened life span and a distinct anatomical distribution of inclusion pathology in the brain of a human A53T transgenic (line M83) mouse. Investigation of α-Syn aggregates in brain stem extracts of end-stage mice demonstrated that the more aggressive phenotype of the α-Syn/p25α strain was associated with an increased load of α-Syn aggregates based on a Förster resonance energy transfer immunoassay and a reduced α-Syn aggregate seeding activity based on a protein misfolding cyclic amplification assay. When injected unilaterally into the striata of wild-type mice, the α-Syn/p25α strain resulted in a more-pronounced motoric phenotype than α-Syn PFF and exhibited a “tropism” for nigro-striatal neurons compared to α-Syn PFF. Overall, our data support a hypothesis whereby oligodendroglial p25α is responsible for generating a highly prodegenerative α-Syn strain in multiple system atrophy.

AB - Pathology consisting of intracellular aggregates of alpha-Synuclein (α-Syn) spread through the nervous system in a variety of neurodegenerative disorders including Parkinson’s disease, dementia with Lewy bodies, and multiple system atrophy. The discovery of structurally distinct α-Syn polymorphs, so-called strains, supports a hypothesis where strain-specific structures are templated into aggregates formed by native α-Syn. These distinct strains are hypothesised to dictate the spreading of pathology in the tissue and the cellular impact of the aggregates, thereby contributing to the variety of clinical phenotypes. Here, we present evidence of a novel α-Syn strain induced by the multiple system atrophy-associated oligodendroglial protein p25α. Using an array of biophysical, biochemical, cellular, and in vivo analyses, we demonstrate that compared to α-Syn alone, a substoichiometric concentration of p25α redirects α-Syn aggregation into a unique α-Syn/p25α strain with a different structure and enhanced in vivo prodegenerative properties. The α-Syn/p25α strain induced larger inclusions in human dopaminergic neurons. In vivo, intramuscular injection of preformed fibrils (PFF) of the α-Syn/p25α strain compared to α-Syn PFF resulted in a shortened life span and a distinct anatomical distribution of inclusion pathology in the brain of a human A53T transgenic (line M83) mouse. Investigation of α-Syn aggregates in brain stem extracts of end-stage mice demonstrated that the more aggressive phenotype of the α-Syn/p25α strain was associated with an increased load of α-Syn aggregates based on a Förster resonance energy transfer immunoassay and a reduced α-Syn aggregate seeding activity based on a protein misfolding cyclic amplification assay. When injected unilaterally into the striata of wild-type mice, the α-Syn/p25α strain resulted in a more-pronounced motoric phenotype than α-Syn PFF and exhibited a “tropism” for nigro-striatal neurons compared to α-Syn PFF. Overall, our data support a hypothesis whereby oligodendroglial p25α is responsible for generating a highly prodegenerative α-Syn strain in multiple system atrophy.

KW - Multiple system atrophy (MSA)

KW - P25α

KW - Protein aggregation

KW - Strains

KW - Tubulin polymerisation-promoting protein (TPPP)

KW - Α-Synuclein

U2 - 10.1007/s00401-021-02316-0

DO - 10.1007/s00401-021-02316-0

M3 - Journal article

C2 - 33978813

AN - SCOPUS:85105889317

SN - 0001-6322

VL - 142

SP - 87

EP - 115

JO - Acta Neuropathologica

JF - Acta Neuropathologica

IS - 1

ER -

Multiple system atrophy-associated oligodendroglial protein p25α stimulates formation of novel α-synuclein strain with enhanced neurodegenerative potential

Abstract

Bibliografisk note

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