Frontotemporal dementia caused by CHMP2B mutation is characterised by neuronal lysosomal storage pathology

FReJA consortium

doi:10.1007/s00401-015-1475-3

Frontotemporal dementia caused by CHMP2B mutation is characterised by neuronal lysosomal storage pathology

FReJA consortium

Basic and Clinical Neuroscience

UCL University College London
University of Cambridge
Neurogenetics Research Laboratory, Department of Neurology, Danish Dementia Research Centre, Rigshospitalet, University of Copenhagen, Copenhagen, Denmark.
Aarhus University
Memory Clinic, Department of Neurology, Danish Dementia Research Centre, Rigshospitalet, University of Copenhagen, Copenhagen, Denmark.
Department of Cellular and Molecular Medicine, Section of Neurogenetics, The Panum Institute, University of Copenhagen, Copenhagen, Denmark.

Research output: Contribution to journal › Article › peer-review

70 Citations (Scopus)

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Abstract

Mutations in the charged multivesicular body protein 2B (CHMP2B) cause frontotemporal dementia (FTD). We report that mice which express FTD-causative mutant CHMP2B at physiological levels develop a novel lysosomal storage pathology characterised by large neuronal autofluorescent aggregates. The aggregates are an early and progressive pathology that occur at 3 months of age and increase in both size and number over time. These autofluorescent aggregates are not observed in mice expressing wild-type CHMP2B, or in non-transgenic controls, indicating that they are a specific pathology caused by mutant CHMP2B. Ultrastructural analysis and immuno- gold labelling confirmed that they are derived from the endolysosomal system. Consistent with these findings, CHMP2B mutation patient brains contain morphologically similar autofluorescent aggregates. These aggregates occur significantly more frequently in human CHMP2B mutation brain than in neurodegenerative disease or age-matched control brains. These data suggest that lysosomal storage pathology is the major neuronal pathology in FTD caused by CHMP2B mutation. Recent evidence suggests that two other genes associated with FTD, GRN and TMEM106B are important for lysosomal function. Our identification of lysosomal storage pathology in FTD caused by CHMP2B mutation now provides evidence that endolysosomal dysfunction is a major degenerative pathway in FTD.

Original language	English
Pages (from-to)	511-523
Number of pages	13
Journal	Acta Neuropathologica
Volume	130
Issue number	4
Early online date	10 Sept 2015
DOIs	https://doi.org/10.1007/s00401-015-1475-3
Publication status	Published - 1 Oct 2015

Keywords

Aged
Aged, 80 and over
Animals
Brain/metabolism
Disease Models, Animal
Disease Progression
Endosomal Sorting Complexes Required for Transport/genetics
Female
Frontotemporal Dementia/genetics
Humans
Lysosomes/metabolism
Male
Mice, Transgenic
Microglia/metabolism
Middle Aged
Mutation
Nerve Tissue Proteins/genetics
Neurons/metabolism
Protein Multimerization

UN SDGs

This output contributes to the following UN Sustainable Development Goals (SDGs)

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10.1007/s00401-015-1475-3Licence: CC BY

Frontotemporal dementia caused by_CLAYTON_Acc2Sept2015Epub10Sept2015_GOLD VoR (CC BY)Accepted author manuscript, 10.9 MBLicence: CC BY

Cite this

@article{95193d7ac278479f930cad763bed08c2,

title = "Frontotemporal dementia caused by CHMP2B mutation is characterised by neuronal lysosomal storage pathology",

abstract = "Mutations in the charged multivesicular body protein 2B (CHMP2B) cause frontotemporal dementia (FTD). We report that mice which express FTD-causative mutant CHMP2B at physiological levels develop a novel lysosomal storage pathology characterised by large neuronal autofluorescent aggregates. The aggregates are an early and progressive pathology that occur at 3 months of age and increase in both size and number over time. These autofluorescent aggregates are not observed in mice expressing wild-type CHMP2B, or in non-transgenic controls, indicating that they are a specific pathology caused by mutant CHMP2B. Ultrastructural analysis and immuno- gold labelling confirmed that they are derived from the endolysosomal system. Consistent with these findings, CHMP2B mutation patient brains contain morphologically similar autofluorescent aggregates. These aggregates occur significantly more frequently in human CHMP2B mutation brain than in neurodegenerative disease or age-matched control brains. These data suggest that lysosomal storage pathology is the major neuronal pathology in FTD caused by CHMP2B mutation. Recent evidence suggests that two other genes associated with FTD, GRN and TMEM106B are important for lysosomal function. Our identification of lysosomal storage pathology in FTD caused by CHMP2B mutation now provides evidence that endolysosomal dysfunction is a major degenerative pathway in FTD. ",

keywords = "Aged, Aged, 80 and over, Animals, Brain/metabolism, Disease Models, Animal, Disease Progression, Endosomal Sorting Complexes Required for Transport/genetics, Female, Frontotemporal Dementia/genetics, Humans, Lysosomes/metabolism, Male, Mice, Transgenic, Microglia/metabolism, Middle Aged, Mutation, Nerve Tissue Proteins/genetics, Neurons/metabolism, Protein Multimerization",

author = "Clayton, {Emma L} and Sarah Mizielinska and Edgar, {James R} and Nielsen, {Troels Tolstrup} and Sarah Marshall and Norona, {Frances E} and Miranda Robbins and Hana Damirji and Holm, {Ida E} and Peter Johannsen and Nielsen, {J{\o}rgen E} and Asante, {Emmanuel A} and John Collinge and {FReJA consortium} and Isaacs, {Adrian M}",

year = "2015",

month = oct,

day = "1",

doi = "10.1007/s00401-015-1475-3",

language = "English",

volume = "130",

pages = "511--523",

journal = "Acta Neuropathologica",

issn = "0001-6322",

publisher = "Springer Verlag",

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TY - JOUR

T1 - Frontotemporal dementia caused by CHMP2B mutation is characterised by neuronal lysosomal storage pathology

AU - Clayton, Emma L

AU - Mizielinska, Sarah

AU - Edgar, James R

AU - Nielsen, Troels Tolstrup

AU - Marshall, Sarah

AU - Norona, Frances E

AU - Robbins, Miranda

AU - Damirji, Hana

AU - Holm, Ida E

AU - Johannsen, Peter

AU - Nielsen, Jørgen E

AU - Asante, Emmanuel A

AU - Collinge, John

AU - FReJA consortium

AU - Isaacs, Adrian M

PY - 2015/10/1

Y1 - 2015/10/1

N2 - Mutations in the charged multivesicular body protein 2B (CHMP2B) cause frontotemporal dementia (FTD). We report that mice which express FTD-causative mutant CHMP2B at physiological levels develop a novel lysosomal storage pathology characterised by large neuronal autofluorescent aggregates. The aggregates are an early and progressive pathology that occur at 3 months of age and increase in both size and number over time. These autofluorescent aggregates are not observed in mice expressing wild-type CHMP2B, or in non-transgenic controls, indicating that they are a specific pathology caused by mutant CHMP2B. Ultrastructural analysis and immuno- gold labelling confirmed that they are derived from the endolysosomal system. Consistent with these findings, CHMP2B mutation patient brains contain morphologically similar autofluorescent aggregates. These aggregates occur significantly more frequently in human CHMP2B mutation brain than in neurodegenerative disease or age-matched control brains. These data suggest that lysosomal storage pathology is the major neuronal pathology in FTD caused by CHMP2B mutation. Recent evidence suggests that two other genes associated with FTD, GRN and TMEM106B are important for lysosomal function. Our identification of lysosomal storage pathology in FTD caused by CHMP2B mutation now provides evidence that endolysosomal dysfunction is a major degenerative pathway in FTD.

AB - Mutations in the charged multivesicular body protein 2B (CHMP2B) cause frontotemporal dementia (FTD). We report that mice which express FTD-causative mutant CHMP2B at physiological levels develop a novel lysosomal storage pathology characterised by large neuronal autofluorescent aggregates. The aggregates are an early and progressive pathology that occur at 3 months of age and increase in both size and number over time. These autofluorescent aggregates are not observed in mice expressing wild-type CHMP2B, or in non-transgenic controls, indicating that they are a specific pathology caused by mutant CHMP2B. Ultrastructural analysis and immuno- gold labelling confirmed that they are derived from the endolysosomal system. Consistent with these findings, CHMP2B mutation patient brains contain morphologically similar autofluorescent aggregates. These aggregates occur significantly more frequently in human CHMP2B mutation brain than in neurodegenerative disease or age-matched control brains. These data suggest that lysosomal storage pathology is the major neuronal pathology in FTD caused by CHMP2B mutation. Recent evidence suggests that two other genes associated with FTD, GRN and TMEM106B are important for lysosomal function. Our identification of lysosomal storage pathology in FTD caused by CHMP2B mutation now provides evidence that endolysosomal dysfunction is a major degenerative pathway in FTD.

KW - Aged

KW - Aged, 80 and over

KW - Animals

KW - Brain/metabolism

KW - Disease Models, Animal

KW - Disease Progression

KW - Endosomal Sorting Complexes Required for Transport/genetics

KW - Female

KW - Frontotemporal Dementia/genetics

KW - Humans

KW - Lysosomes/metabolism

KW - Male

KW - Mice, Transgenic

KW - Microglia/metabolism

KW - Middle Aged

KW - Mutation

KW - Nerve Tissue Proteins/genetics

KW - Neurons/metabolism

KW - Protein Multimerization

U2 - 10.1007/s00401-015-1475-3

DO - 10.1007/s00401-015-1475-3

M3 - Article

C2 - 26358247

SN - 0001-6322

VL - 130

SP - 511

EP - 523

JO - Acta Neuropathologica

JF - Acta Neuropathologica

IS - 4

ER -

Frontotemporal dementia caused by CHMP2B mutation is characterised by neuronal lysosomal storage pathology

Abstract

Keywords

UN SDGs

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