Cellular, molecular and functional characterisation of YAC transgenic mouse models of Friedreich Ataxia

A Wong; AH Koeppen; AH Koeppen; Annalisa Pastore; B Tomassini; C Sandi; C Sandi; CH Miller; Chiranjeevi Sandi; CJ Miranda; D Waldvogel; F Foury; H Puccio; HA Young; J Gerber; JH Willis; JL Bradley; JM Gottesfeld; JP Sarsero; M Cnop; M Pandolfo; M Pandolfo; M Ristow; MA Pook; Mark A. Pook; RM Clark; S Al-Mahdawi; S Al-Mahdawi; S Al-Mahdawi; Sahar Al-Mahdawi; Sara Anjomani Virmouni; V Campuzano; V Campuzano; Y Shan

research

Cellular, molecular and functional characterisation of YAC transgenic mouse models of Friedreich Ataxia

Authors: A Wong
AH Koeppen
AH Koeppen
Annalisa Pastore
B Tomassini
C Sandi
C Sandi
CH Miller
Chiranjeevi Sandi
CJ Miranda
D Waldvogel
F Foury
H Puccio
HA Young
J Gerber
JH Willis
JL Bradley
JM Gottesfeld
JP Sarsero
M Cnop
M Pandolfo
M Pandolfo
M Ristow
MA Pook
Mark A. Pook
RM Clark
S Al-Mahdawi
S Al-Mahdawi
S Al-Mahdawi
Sahar Al-Mahdawi
Sara Anjomani Virmouni
V Campuzano
V Campuzano
Y Shan
Publication date: 1 January 2014
Publisher: 'Public Library of Science (PLoS)'
Doi

Abstract

Copyright © 2014 Anjomani Virmouni et al. This is an open-access article distributed under the terms of the Creative Commons Attribution License, which permits unrestricted use, distribution, and reproduction in any medium, provided the original author and source are credited.This article has been made available through the Brunel Open Access Publishing Fund.Background - Friedreich ataxia (FRDA) is an autosomal recessive neurodegenerative disorder, caused by a GAA repeat expansion mutation within intron 1 of the FXN gene. We have previously established and performed preliminary characterisation of several human FXN yeast artificial chromosome (YAC) transgenic FRDA mouse models containing GAA repeat expansions, Y47R (9 GAA repeats), YG8R (90 and 190 GAA repeats) and YG22R (190 GAA repeats). Methodology/Principal Findings - We now report extended cellular, molecular and functional characterisation of these FXN YAC transgenic mouse models. FXN transgene copy number analysis of the FRDA mice demonstrated that the YG22R and Y47R lines each have a single copy of the FXN transgene while the YG8R line has two copies. Single integration sites of all transgenes were confirmed by fluorescence in situ hybridisation (FISH) analysis of metaphase and interphase chromosomes. We identified significant functional deficits, together with a degree of glucose intolerance and insulin hypersensitivity, in YG8R and YG22R FRDA mice compared to Y47R and wild-type control mice. We also confirmed increased somatic GAA repeat instability in the cerebellum and brain of YG22R and YG8R mice, together with significantly reduced levels of FXN mRNA and protein in the brain and liver of YG8R and YG22R compared to Y47R. Conclusions/Significance - Together these studies provide a detailed characterisation of our GAA repeat expansion-based YAC transgenic FRDA mouse models that will help investigations of FRDA disease mechanisms and therapy.European Union, Ataxia UK and FARA