Exome sequencing identifies a missense mutation in Isl1 associated with low penetrance otitis media in dearisch mice

Inflammation of the middle ear (otitis media) is very common and can lead to serious complications if not resolved. Genetic studies suggest an inherited component, but few of the genes that contribute to this condition are known. Mouse mutants have contributed significantly to the identification of...

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Published in:Genome biology 2011-09, Vol.12 (9), p.R90-R90
Main Authors: Hilton, Jennifer M, Lewis, Morag A, Grati, M'hamed, Ingham, Neil, Pearson, Selina, Laskowski, Roman A, Adams, David J, Steel, Karen P
Format: Article
Language:English
Subjects:
Animals
Ear, Middle - pathology
Ethylnitrosourea - adverse effects
Evoked Potentials, Auditory, Brain Stem
Exome
Female
Genetic Predisposition to Disease
Immunohistochemistry
Inbreeding
LIM-Homeodomain Proteins - genetics
Male
Mice
Mice, Inbred C3H
Mice, Inbred C57BL
Mutation, Missense
Otitis Media - genetics
Pedigree
Penetrance
Point Mutation
Protein Structure, Secondary
Sequence Analysis, DNA
Transcription Factors - genetics
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Summary:Inflammation of the middle ear (otitis media) is very common and can lead to serious complications if not resolved. Genetic studies suggest an inherited component, but few of the genes that contribute to this condition are known. Mouse mutants have contributed significantly to the identification of genes predisposing to otitis media The dearisch mouse mutant is an ENU-induced mutant detected by its impaired Preyer reflex (ear flick in response to sound). Auditory brainstem responses revealed raised thresholds from as early as three weeks old. Pedigree analysis suggested a dominant but partially penetrant mode of inheritance. The middle ear of dearisch mutants shows a thickened mucosa and cellular effusion suggesting chronic otitis media with effusion with superimposed acute infection. The inner ear, including the sensory hair cells, appears normal. Due to the low penetrance of the phenotype, normal backcross mapping of the mutation was not possible. Exome sequencing was therefore employed to identify a non-conservative tyrosine to cysteine (Y71C) missense mutation in the Islet1 gene, Isl1(Drsh). Isl1 is expressed in the normal middle ear mucosa. The findings suggest the Isl1(Drsh) mutation is likely to predispose carriers to otitis media. Dearisch, Isl1(Drsh), represents the first point mutation in the mouse Isl1 gene and suggests a previously unrecognized role for this gene. It is also the first recorded exome sequencing of the C3HeB/FeJ background relevant to many ENU-induced mutants. Most importantly, the power of exome resequencing to identify ENU-induced mutations without a mapped gene locus is illustrated.
ISSN:1465-6906
1474-760X
1465-6914
DOI:10.1186/gb-2011-12-9-r90