Reversal of pathology in CHMP2B-mediated frontotemporal dementia patient cells using RNA interference

Troels Tolstrup Nielsen; Sarah Mizielinska; Lis Hasholt; Adrian M Isaacs; Jørgen E Nielsen; the FReJA Consortium

doi:10.1002/jgm.2649

Reversal of pathology in CHMP2B-mediated frontotemporal dementia patient cells using RNA interference

Troels Tolstrup Nielsen, Sarah Mizielinska, Lis Hasholt, Adrian M Isaacs, Jørgen E Nielsen, the FReJA Consortium

12 Citations (Scopus)

Abstract

Background: Frontotemporal dementia is the second most common form of young-onset dementia after Alzheimer's disease, and several genetic forms of frontotemporal dementia are known. A rare genetic variant is caused by a point mutation in the CHMP2B gene. CHMP2B is a component of the ESCRT-III complex, which is involved in endosomal trafficking of proteins targeted for degradation in lysosomes. Mutations in CHMP2B result in abnormal endosomal structures in patient fibroblasts and patient brains, probably through a gain-of-function mechanism, suggesting that the endosomal pathway plays a central role in the pathogenesis of the disease. Methods: In the present study, we used lentiviral vectors to efficiently knockdown CHMP2B by delivering microRNA embedded small hairpin RNAs. Results: We show that CHMP2B can be efficiently knocked down in patient fibroblasts using an RNA interference approach and that the knockdown causes reversal of the abnormal endosomal phenotype observed in patient fibroblasts. Conclusions: This is the first description of a treatment that reverses the cellular pathology caused by mutant CHMP2B and suggests that RNA interference might be a feasible therapeutic strategy. Furthermore, it provides the first proof of a direct link between the disease-causing mutation and the cellular phenotype in cells originating from CHMP2B mutation patients.

Original language	English
Journal	Journal of Gene Medicine
Volume	14
Issue number	8
Pages (from-to)	521-529
Number of pages	9
ISSN	1099-498X
DOIs	https://doi.org/10.1002/jgm.2649
Publication status	Published - Aug 2012

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@article{3d7013aca7fb4af998adc9e9aa0f7fff,

title = "Reversal of pathology in CHMP2B-mediated frontotemporal dementia patient cells using RNA interference",

abstract = "Background: Frontotemporal dementia is the second most common form of young-onset dementia after Alzheimer's disease, and several genetic forms of frontotemporal dementia are known. A rare genetic variant is caused by a point mutation in the CHMP2B gene. CHMP2B is a component of the ESCRT-III complex, which is involved in endosomal trafficking of proteins targeted for degradation in lysosomes. Mutations in CHMP2B result in abnormal endosomal structures in patient fibroblasts and patient brains, probably through a gain-of-function mechanism, suggesting that the endosomal pathway plays a central role in the pathogenesis of the disease. Methods: In the present study, we used lentiviral vectors to efficiently knockdown CHMP2B by delivering microRNA embedded small hairpin RNAs. Results: We show that CHMP2B can be efficiently knocked down in patient fibroblasts using an RNA interference approach and that the knockdown causes reversal of the abnormal endosomal phenotype observed in patient fibroblasts. Conclusions: This is the first description of a treatment that reverses the cellular pathology caused by mutant CHMP2B and suggests that RNA interference might be a feasible therapeutic strategy. Furthermore, it provides the first proof of a direct link between the disease-causing mutation and the cellular phenotype in cells originating from CHMP2B mutation patients.",

author = "Nielsen, {Troels Tolstrup} and Sarah Mizielinska and Lis Hasholt and Isaacs, {Adrian M} and Nielsen, {J{\o}rgen E} and {the FReJA Consortium}",

note = "Copyright {\textcopyright} 2012 John Wiley & Sons, Ltd.",

year = "2012",

month = aug,

doi = "10.1002/jgm.2649",

language = "English",

volume = "14",

pages = "521--529",

journal = "Journal of Gene Medicine",

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number = "8",

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T1 - Reversal of pathology in CHMP2B-mediated frontotemporal dementia patient cells using RNA interference

AU - Nielsen, Troels Tolstrup

AU - Mizielinska, Sarah

AU - Hasholt, Lis

AU - Isaacs, Adrian M

AU - Nielsen, Jørgen E

AU - the FReJA Consortium

PY - 2012/8

Y1 - 2012/8

N2 - Background: Frontotemporal dementia is the second most common form of young-onset dementia after Alzheimer's disease, and several genetic forms of frontotemporal dementia are known. A rare genetic variant is caused by a point mutation in the CHMP2B gene. CHMP2B is a component of the ESCRT-III complex, which is involved in endosomal trafficking of proteins targeted for degradation in lysosomes. Mutations in CHMP2B result in abnormal endosomal structures in patient fibroblasts and patient brains, probably through a gain-of-function mechanism, suggesting that the endosomal pathway plays a central role in the pathogenesis of the disease. Methods: In the present study, we used lentiviral vectors to efficiently knockdown CHMP2B by delivering microRNA embedded small hairpin RNAs. Results: We show that CHMP2B can be efficiently knocked down in patient fibroblasts using an RNA interference approach and that the knockdown causes reversal of the abnormal endosomal phenotype observed in patient fibroblasts. Conclusions: This is the first description of a treatment that reverses the cellular pathology caused by mutant CHMP2B and suggests that RNA interference might be a feasible therapeutic strategy. Furthermore, it provides the first proof of a direct link between the disease-causing mutation and the cellular phenotype in cells originating from CHMP2B mutation patients.

AB - Background: Frontotemporal dementia is the second most common form of young-onset dementia after Alzheimer's disease, and several genetic forms of frontotemporal dementia are known. A rare genetic variant is caused by a point mutation in the CHMP2B gene. CHMP2B is a component of the ESCRT-III complex, which is involved in endosomal trafficking of proteins targeted for degradation in lysosomes. Mutations in CHMP2B result in abnormal endosomal structures in patient fibroblasts and patient brains, probably through a gain-of-function mechanism, suggesting that the endosomal pathway plays a central role in the pathogenesis of the disease. Methods: In the present study, we used lentiviral vectors to efficiently knockdown CHMP2B by delivering microRNA embedded small hairpin RNAs. Results: We show that CHMP2B can be efficiently knocked down in patient fibroblasts using an RNA interference approach and that the knockdown causes reversal of the abnormal endosomal phenotype observed in patient fibroblasts. Conclusions: This is the first description of a treatment that reverses the cellular pathology caused by mutant CHMP2B and suggests that RNA interference might be a feasible therapeutic strategy. Furthermore, it provides the first proof of a direct link between the disease-causing mutation and the cellular phenotype in cells originating from CHMP2B mutation patients.

U2 - 10.1002/jgm.2649

DO - 10.1002/jgm.2649

M3 - Journal article

C2 - 22786763

SN - 1099-498X

VL - 14

SP - 521

EP - 529

JO - Journal of Gene Medicine

JF - Journal of Gene Medicine

IS - 8

ER -

Reversal of pathology in CHMP2B-mediated frontotemporal dementia patient cells using RNA interference

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