Frataxin knockin mouse

Top Cited Papers

18 January 2002

journal article
Published by Wiley

Vol. 512 (1-3) , 291-297
https://doi.org/10.1016/s0014-5793(02)02251-2

Abstract

Friedreich ataxia is the consequence of frataxin deficiency, most often caused by a GAA repeat expansion in intron 1 of the corresponding gene. Frataxin is a mitochondrial protein involved in iron homeostasis. As an attempt to generate a mouse model of the disease, we introduced a (GAA)₂₃₀ repeat within the mouse frataxin gene by homologous recombination. GAA repeat knockin mice were crossed with frataxin knockout mice to obtain double heterozygous mice expressing 25–36% of wild-type frataxin levels. These mice were viable and did not develop anomalies of motor coordination, iron metabolism or response to iron loading. Repeats were meiotically and mitotically stable.

Keywords

This publication has 29 references indexed in Scilit:

Friedreich ataxia: an overview
Journal of Medical Genetics, 2000
Studies of human, mouse and yeast homologues indicate a mitochondrial function for frataxin
Nature Genetics, 1997
Phenotype Correlation and Intergenerational Dynamics of the Friedreich Ataxia GAA Trinucleotide Repeat
American Journal of Human Genetics, 1997
Regulation of Mitochondrial Iron Accumulation by Yfh1p, a Putative Homolog of Frataxin
Science, 1997
Phenotypic variability in friedreich ataxia: Role of the associated GAA triplet repeat expansion
Annals of Neurology, 1997
Development of a sensitive reverse transcriptase PCR assay, RT-RPCR, utilizing rapid cycle times.
Genome Research, 1992
Friedreich's ataxia: a descriptive epidemiological study in an Italian population
Clinical Genetics, 1990
The heart in Friedreich's ataxia.
Journal of Neurology, Neurosurgery & Psychiatry, 1983
CLASSIFICATION OF THE HEREDITARY ATAXIAS AND PARAPLEGIAS
The Lancet, 1983
FRIEDREICH'S ATAXIA: A CLINICAL AND GENETIC STUDY OF 90 FAMILIES WITH AN ANALYSIS OF EARLY DIAGNOSTIC CRITERIA AND INTRAFAMILIAL CLUSTERING OF CLINICAL FEATURES
Brain, 1981