2019
DOI: 10.3389/fnins.2019.01255
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A Novel Mouse Model of MYO7A USH1B Reveals Auditory and Visual System Haploinsufficiencies

Abstract: Usher’s syndrome is the most common combined blindness–deafness disorder with USH1B, caused by mutations in MYO7A, resulting in the most severe phenotype. The existence of numerous, naturally occurring shaker1 mice harboring variable MYO7A mutations on different genetic backgrounds has complicated the characterization of MYO7A knockout (KO) and heterozygote mice. We generated a novel MYO7A KO mouse (Myo7a–/–) that is easily genotyped, maintained, and confirmed to be null for MYO7A in both the eye and inner ear… Show more

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Cited by 21 publications
(13 citation statements)
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“…Specifically, although some deficiencies in vision have been reported, no mouse mutant has shown retinal degeneration/morphology defects unless exposed to altered light conditions (i.e. enhanced light/lack of pigmentation) ( Calabro et al, 2019 ; Haywood-Watson et al, 2006 ; Lentz et al, 2010 ; Libby and Steel, 2001 ; Libby et al, 2003 ; Peng et al, 2011 ; Trouillet et al, 2018 ; Williams et al, 2009 ). One possible explanation is that mice exhibit a photoreceptor structure that diverges from that of humans and other species ( El-Amraoui and Petit, 2014 ).…”
Section: Introductionmentioning
confidence: 99%
“…Specifically, although some deficiencies in vision have been reported, no mouse mutant has shown retinal degeneration/morphology defects unless exposed to altered light conditions (i.e. enhanced light/lack of pigmentation) ( Calabro et al, 2019 ; Haywood-Watson et al, 2006 ; Lentz et al, 2010 ; Libby and Steel, 2001 ; Libby et al, 2003 ; Peng et al, 2011 ; Trouillet et al, 2018 ; Williams et al, 2009 ). One possible explanation is that mice exhibit a photoreceptor structure that diverges from that of humans and other species ( El-Amraoui and Petit, 2014 ).…”
Section: Introductionmentioning
confidence: 99%
“…Found on chromosome 11, the MYO7A gene encodes for a 250 kDa unconventional myosin that contains an N-terminal canonical myosin motor domain with a high duty ratio, five light-chain binding IQ motifs, and two MyTH4/FERM domains in its tail region, separated by an SH3 domain ( Figure 2 ; El-Amraoui et al, 2008 ; Heissler and Manstein, 2012 ). Due to its expression in both the calyceal processes and stereocilia, MYO7A mutations have been associated with both vision and hearing loss ( Calabro et al, 2019 ). Two distinct modes of hearing loss are commonly associated with MYO7A mutations, known as DFNA11 and DFNB2.…”
Section: The Myosin Superfamilymentioning
confidence: 99%
“…A mouse model of USH1B, known as shaker-1, contains a mutation in the MYO7A gene and displays both vision and hearing loss phenotypes ( Eudy and Sumegi, 1999 ). Interestingly, MYO7A (–/–) mice with no MYO7A expression have profound hearing and vision loss, displaying a loss of both inner and outer hair cells, though no loss in calyceal process structure or photoreceptor cells ( Calabro et al, 2019 ).…”
Section: The Myosin Superfamilymentioning
confidence: 99%
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“…Ewaso mice have the mutation p.I487N and have abnormal vestibular hair cells (Calabro et al, 2019). Dumbo mice have the mutation p.F947I and exhibit disorganized cochlear hair cells during development (Miller et al, 2012).…”
Section: Animal Modelsmentioning
confidence: 99%