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Biallelic mutations in SNX14 cause a syndromic form of cerebellar atrophy and lysosome-autophagosome dysfunction.

Pediatric-onset ataxias often present clinically as developmental delay and intellectual disability, with prominent cerebellar atrophy as a key neuroradiographic finding. Here we describe a new clinically distinguishable recessive syndrome in 12 families with cerebellar atrophy together with ataxia, coarsened facial features and intellectual disability, due to truncating mutations in the sorting nexin gene SNX14, encoding a ubiquitously expressed modular PX domain-containing sorting factor. We found SNX14 localized to lysosomes and associated with phosphatidylinositol (3,5)-bisphosphate, a key component of late endosomes/lysosomes. Patient-derived cells showed engorged lysosomes and a slower autophagosome clearance rate upon autophagy induction by starvation. Zebrafish morphants for snx14 showed dramatic loss of cerebellar parenchyma, accumulation of autophagosomes and activation of apoptosis. Our results characterize a unique ataxia syndrome due to biallelic SNX14 mutations leading to lysosome-autophagosome dysfunction

eScholarship - University of California

Biallelic Mutations in Snx14 Cause A Syndromic Form of Cerebellar Atrophy and Lysosome-Autophagosome Dysfunction

Author: A Deik
A Heiseke
Abdelrahim A Sadek
AC Thomas
Ali Dursun
Amera El Badawy
Amira Masri
Antoinette Bernabe Gelot
Ashleigh E Schaffer
Basak Rosti
Brett Copeland
C Dall′Armi
CS Chen
DC Ko
E Wong
Eric M Scott
Esra Dikoglu
Faezeh Mojahedi
Gennaro Napolitano
Ghada M Abdel-Salam
HC Dippold
HS Huang
Hulya Kayserili
Iman G Mahmoud
Isabelle Desguerre
J Lee
J Lim
Jana Schroth
Jean-Laurent Casanova
Jeffrey D Esko
Jennifer L Silhavy
JM Hegarty
Joseph G Gleeson
JP Taylor
JW Lin
K Bilguvar
K Okita
Keith K Vaux
KL Meerbrey
L Paton
Laila Bastaki
Laila Selim
Lihadh Al-Gazali
M Aker
M Fromer
M Gallon
M Komatsu
MA DePristo
Maha S Zaki
Mahmut Samil Sagıroglu
Matloob Azam
Matthew D Buschman
MC Marchetto
Mona Aglan
Murat Gunel
N Raben
Naiara Akizu
O Pampliega
P Coutinho
Pascale de Lonlay
Philip L S M Gordts
PL Gordts
R Bargal
R Koksal Ozgul
Rasim Ozgur Rosti
RH Roda
Samia Temtamy
Samira Ismail
Sawsan Abdel-Hadi
SB Sousa
Seth J Field
Stacey B Gabriel
T Cullup
T Hara
TJ Dixon-Salazar
Ulrich Müller
Vincent Cantagrel
X Wang
Xin Wang
Y Batlevi
Y Zhao
Publication venue: 'Springer Science and Business Media LLC'
Publication date: 01/01/2015
Field of study

Pediatric-onset ataxias often present clinically with developmental delay and intellectual disability, with prominent cerebellar atrophy as a key neuroradiographic finding. Here we describe a novel clinically distinguishable recessive syndrome in 12 families with cerebellar atrophy together with ataxia, coarsened facial features and intellectual disability, due to truncating mutations in sorting nexin 14 (SNX14), encoding a ubiquitously expressed modular PX-domain-containing sorting factor. We found SNX14 localized to lysosomes, and associated with phosphatidyl-inositol (3,5)P2, a key component of late endosomes/lysosomes. Patient cells showed engorged lysosomes and slower autophagosome clearance rate upon starvation induction. Zebrafish morphants showed dramatic loss of cerebellar parenchyma, accumulated autophagosomes, and activation of apoptosis. Our results suggest a unique ataxia syndrome due to biallelic SNX14 mutations, leading to lysosome-autophagosome dysfunction.PubMedWo

Hacettepe University Institutional Repository

Archivio della ricerca - Università degli studi di Napoli Federico II

Crossref

PubMed Central

eScholarship - University of California

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