p53 is a central regulator driving neurodegeneration caused by C9orf72 poly(PR)

M. Maor-Nof; Z. Shipony; R. Lopez-Gonzalez; L. Nakayama; Y.-J. Zhang; J. Couthouis; J.A. Blum; P.A. Castruita; G.R. Linares; K. Ruan; G. Ramaswami; D.J. Simon; A. Nof; M. Santana; K. Han; N. Sinnott-Armstrong; M.C. Bassik; D.H. Geschwind; M. Tessier-Lavigne; L.D. Attardi; T.E. Lloyd; J.K. Ichida; F.-B. Gao; W.J. Greenleaf; J.S. Yokoyama; L. Petrucelli; A.D. Gitler

doi:10.1016/j.cell.2020.12.025

Journal article

p53 is a central regulator driving neurodegeneration caused by C9orf72 poly(PR)

M. Maor-Nof, Z. Shipony, R. Lopez-Gonzalez, L. Nakayama, Y.-J. Zhang, J. Couthouis, J.A. Blum, P.A. Castruita, G.R. Linares, K. Ruan, …

Cell, Vol.184(3), p.689

2021

DOI: https://doi.org/10.1016/j.cell.2020.12.025

PMID: 33482083

Abstract

Animals

Apoptosis Regulatory Proteins

Axons

C9orf72 Protein

Cell Death

Cells, Cultured

Cerebral Cortex

Chromatin

Disease Models, Animal

DNA Damage

DNA Repeat Expansion

Drosophila

Mice, Inbred C57BL

Nerve Degeneration

Protein Stability

Transcription, Genetic

Tumor Suppressor Protein p53

Tumor Suppressor Proteins

dipeptide

poly(glycine arginine)

poly(proline arginine)

protein p53

PUMA protein

small interfering RNA

unclassified drug

apoptosis regulatory protein

axon

guanine nucleotide exchange C9orf72

protein p53

PUMA protein, mouse

repetitive DNA

tumor suppressor protein

amyotrophic lateral sclerosis

animal cell

animal experiment

animal model

animal tissue

Article

brain nerve cell

C9orf72 gene

cell survival

chromatin

comet assay

controlled study

CRISPR-CAS9 system

Drosophila

embryo

female

frontotemporal dementia

gene

HEK293T cell line

histology

immunoblotting

immunocytochemistry

in vitro study

induced pluripotent stem cell

male

mouse

nerve cell differentiation

nerve degeneration

nonhuman

RNA sequence

sequence analysis

spinal cord

survival

animal

brain cortex

C57BL mouse

cell culture

cell death

disease model

DNA damage

genetic transcription

genetics

metabolism

nerve degeneration

pathology

protein stability

The most common genetic cause of amyotrophic lateral sclerosis (ALS) and frontotemporal dementia (FTD) is a GGGGCC repeat expansion in the C9orf72 gene. We developed a platform to interrogate the chromatin accessibility landscape and transcriptional program within neurons during degeneration. We provide evidence that neurons expressing the dipeptide repeat protein poly(proline-arginine), translated from the C9orf72 repeat expansion, activate a highly specific transcriptional program, exemplified by a single transcription factor, p53. Ablating p53 in mice completely rescued neurons from degeneration and markedly increased survival in a C9orf72 mouse model. p53 reduction also rescued axonal degeneration caused by poly(glycine-arginine), increased survival of C9orf72 ALS/FTD-patient-induced pluripotent stem cell (iPSC)-derived motor neurons, and mitigated neurodegeneration in a C9orf72 fly model. We show that p53 activates a downstream transcriptional program, including Puma, which drives neurodegeneration. These data demonstrate a neurodegenerative mechanism dynamically regulated through transcription-factor-binding events and provide a framework to apply chromatin accessibility and transcription program profiles to neurodegeneration. © 2020 Elsevier Inc.; C9orf72 mutations associated with ALS and FTD activate a specific transcriptional program that converges on p53 to drive neurodegeneration in multiple C9orf72 models. © 2020 Elsevier Inc.

Files and links (1)

url

https://www.scopus.com/inward/record.uri?eid=2-s2.0-85100427326&doi=10.1016%2fj.cell.2020.12.025&partnerID=40&md5=83165aa4965249173e1fe561c0d6fd27View

Metrics

1 Record Views

See more details

Details

Title: p53 is a central regulator driving neurodegeneration caused by C9orf72 poly(PR)
Creators: M. Maor-Nof - Stanford University
Z. Shipony - Stanford University
R. Lopez-Gonzalez
L. Nakayama - Stanford University
Y.-J. Zhang - Mayo Clinic in Florida
J. Couthouis - Stanford University
J.A. Blum - Stanford University
P.A. Castruita - University Memory and Aging Center
G.R. Linares - University of Southern California
K. Ruan - Johns Hopkins University
G. Ramaswami - University of California, Los Angeles
D.J. Simon - Stanford University
A. Nof - Stanford University
M. Santana - Broad Center
K. Han - Stanford University
N. Sinnott-Armstrong - Stanford University
M.C. Bassik - Stanford University
D.H. Geschwind - University of California, Los Angeles
M. Tessier-Lavigne - Stanford University
L.D. Attardi - Stanford University
T.E. Lloyd - Johns Hopkins University
J.K. Ichida - Broad Center
F.-B. Gao - University of Massachusetts Chan Medical School
W.J. Greenleaf - Stanford University
J.S. Yokoyama - University of California, San Francisco
L. Petrucelli - Mayo Clinic in Florida
A.D. Gitler - Stanford University
Publication Details: Cell, Vol.184(3), p.689
Publisher: Elsevier B.V.; CAMBRIDGE
Number of pages: 40
Grant note: National Institutes of Health [NIH]: NS069375 EMBO long-term fellowship: ALTF 301-2017 SSSI-Muscular Dystrophy AssociationStanford School of Medicine Dean's postdoctoral fellowshipsNIH: S10OD020141, R35NS097263(10), R01NS094239, R01NS101986, R37NS057553, R35NS097273(17), P01NS084974 Target ALSBlavatnik Family FoundationAlzheimer's Association: 2018-AARFD-592264 Brain Rejuvenation Project of the Wu Tsai Neurosciences InstituteU.S. Department of Defense: W81XWH-15-1-0187 Merkin Family FoundationNew York Stem Cell FoundationJohn Douglas French Alzheimer's FoundationTau ConsortiumStanford UniversityStanford Research Computing CenterThe NIH: P01NS099114, R01NS089786, 1F32MH114620, K01AG049152, R35CA197591, R01MH109912, R01NS097850, R01NS097850-01S1, P50HG007735, R01HG008140, U19AI057266, UM1HG009442, 1UM1HG009436 National Cancer Institute: R35CA197591 National Human Genome Research Institute: R01HG008140, RM1HG007735 National Institute of Allergy and Infectious Diseases: U19AI057266 National Institute of Neurological Disorders and Stroke: R35NS097263, P01NS099114, R37NS057553, R35NS097273 National Institute of Neurological Disorders and Stroke; National Institute on Aging: R01NS101986 National Institute of Neurological Disorders and Stroke; National Institute on Aging: R01NS097850 National Institute on Aging: P01AG019724, P01NS084974
We thank Dr. Andrew Olson (Stanford Neuroscience Microscopy Service, supported by National Institutes of Health [NIH] grant NS069375). M.M.-N. is supported by an EMBO long-term fellowship (ALTF 301-2017), the SSSI-Muscular Dystrophy Association (M.M.-N.), and Stanford School of Medicine Dean's postdoctoral fellowships (M.M.-N.). This work was supported by NIH grants R35NS097263(10) (A.D.G.), R01NS094239 (T.E.L.), R01NS101986 (F.-B.G.), R37NS057553 (F.-B.G.), R35NS097273(17) (L.P.), P01NS084974 (L.P.), P01NS099114 (L.P.), R01NS089786 (M.T.L.), 1F32MH114620 (G.R.), K01AG049152 (J.S.Y.), R35CA197591 (L.D.A.), R01MH109912 (D.H.G.), R01NS097850 (J.K.I.), R01NS097850-01S1 (R.L.-G.), P50HG007735 (W.J.G.), R01HG008140 (W.J.G.), U19AI057266 (W.J.G.), UM1HG009442 (W.J.G.), and 1UM1HG009436 (W.J.G.); the Robert Packard Center for ALS Research at Johns Hopkins (A.D.G.); Target ALS (A.D.G., F.-B.G., J.C., L.P., and T.E.L.); the Blavatnik Family Foundation (J.A.B.); the Alzheimer's Association (2018-AARFD-592264 to G.R.L.); the Brain Rejuvenation Project of the Wu Tsai Neurosciences Institute (A.D.G.); the U.S. Department of Defense (grant W81XWH-15-1-0187 to J.K.I.); the Merkin Family Foundation (J.K.I.); the New York Stem Cell Foundation (J.K.I.); the John Douglas French Alzheimer's Foundation; and the Tau Consortium (J.K.I.). J.K.I. is a New York Stem Cell Foundation Robertson Investigator and a Richard N. Merkin Scholar. W.J.G. is a Chan Zuckerberg Biohub investigator. Some of the computing for this project was performed on the Sherlock cluster. We would like to thank Stanford University and the Stanford Research Computing Center for providing computational resources and support that contributed to these research results. This work used the Genome Sequencing Service Center by Stanford Center for Genomics and Personalized Medicine Sequencing Center, supported by NIH grant S10OD020141. Some of the figures were created with BioRender.com.
Comment: Export Date: 27 February 2026; Cited By: 128; CODEN: CELLB
Academic Unit: Level 02 - Executives; Executives; UMMG Department of Neurology
Resource Type: Journal article
PMID: 33482083
Record Identifier: 991032996201602976