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Inactivation of CDK/pRb Pathway Normalizes Survival Pattern of Lymphoblasts Expressing the FTLD-Progranulin Mutation c.709-1G>A

Author: A Appert-Collin
A Capell
A Cossarizza
A Eckert
A Gladkevich
A Guo
A Lopez de Munain
A Ricobaraza
A Samali
Adolfo López de Munain
Ainhoa Alzualde
B Cenik
B Langley
B Mosch
C Alquezar
C Brodski
Carolina Alquezar
D Dormann
D Ibarreta
D Uberti
D Uberti
DS Park
DX Liu
E Bialopiotrowicz
E Cova
E Menu
EY Rosen
F Bartolome
F Hu
F Moreno
Fermín Moreno
G Koh
GM McKhann
GU Hoglinger
H Ino
H Osuga
HJ Kim
I Nicoletti
IR Mackenzie
IR Mackenzie
J Naderi
J Ruffels
J Stieler
JL Eriksen
JW Husseman
K Hernandez-Ortega
K Herrup
KA Vassall
Kelly Jordan-Sciutto
L Li
LA Greene
LM Igaz
M Baker
M Cruts
M Kamrava
Matilde S. Ayuso
MD Nguyen
MR Jeong
MS Forman
N Mitsiades
NJ Cairns
NJ Cairns
Noemí Esteras
P Bossu
P Gallinari
P Koistinen
P Van Damme
R Daniel
RR Guerra
S Harguindey
SG Sala
SK Kidd
ST DeKosky
T Zanocco-Marani
U Munoz
W Tang
YJ Zhang
YM Ayala
Z Nagy
Ángeles Martín-Requero
Publication venue: Public Library of Science
Publication date: 18/05/2012
Field of study

8 figuras, 2 tablasBackground Mutations in the progranulin (PGRN) gene, leading to haploinsufficiency, cause familial frontotemporal lobar degeneration (FTLD-TDP), although the pathogenic mechanism of PGRN deficit is largely unknown. Allelic loss of PGRN was previously shown to increase the activity of cyclin-dependent kinase (CDK) CDK6/pRb pathway in lymphoblasts expressing the c.709-1G>A PGRN mutation. Since members of the CDK family appear to play a role in neurodegenerative disorders and in apoptotic death of neurons subjected to various insults, we investigated the role of CDK6/pRb in cell survival/death mechanisms following serum deprivation. Methodology/Principal Findings We performed a comparative study of cell viability after serum withdrawal of established lymphoblastoid cell lines from control and carriers of c.709-1G>A PGRN mutation, asymptomatic and FTLD-TDP diagnosed individuals. Our results suggest that the CDK6/pRb pathway is enhanced in the c.709-1G>A bearing lymphoblasts. Apparently, this feature allows PGRN-deficient cells to escape from serum withdrawal-induced apoptosis by decreasing the activity of executive caspases and lowering the dissipation of mitochondrial membrane potential and the release of cytochrome c from the mitochondria. Inhibitors of CDK6 expression levels like sodium butyrate or the CDK6 activity such as PD332991 were able to restore the vulnerability of lymphoblasts from FTLD-TDP patients to trophic factor withdrawal. Conclusion/Significance The use of PGRN-deficient lymphoblasts from FTLD-TDP patients may be a useful model to investigate cell biochemical aspects of this disease. It is suggested that CDK6 could be potentially a therapeutic target for the treatment of the FTLD-TDPThis work has been supported by grants from Ministry of Education and Science (SAF2007-61701, SAF2010-15700, SAF2011-28603), Fundación Eugenio Rodríguez Pascual, and Basque Government (Saiotek program 2008–2009). NE holds a fellowship of the JAE predoctoral program of the CSICPeer reviewe

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