Auditory function and hearing loss in children and adults with Williams syndrome: Cochlear impairment in individuals with otherwise normal hearing

Marler, Jeffrey A.; Sitcovsky, Jessica L.; Mervis, Carolyn Β.; Kistler, Doris J.; Wightman, Frederic L.

doi:10.1002/ajmg.c.30262

Cited by 38 publications

(62 citation statements)

References 91 publications

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“…Adults typically have a stiff awkward gait characterized by reduced speed and stride length [Hocking et al, 2009]. Sensorineural hearing loss is common in both children and adults, and many are noted to be hypersensitive to sound [Gothelf et al, 2006;Marler et al, 2010]. Advances in neuroimaging techniques show subtle structural differences in WS.…”

Section: Central Neurologic Signs and Neuroanatomymentioning

confidence: 99%

The behavioral phenotype of Williams syndrome: A recognizable pattern of neurodevelopment

Morris

2010

American J of Med Genetics Pt C

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Williams syndrome (WS), caused by hemizygous deletion of 1.55-1.8 Mb of chromosome 7q11.23, has a recognizable behavior phenotype that is an important diagnostic sign. Individuals with WS are overly friendly, gregarious, empathetic, and loquacious, but have difficulty interpreting social cues and in making and keeping friends. The neurodevelopmental profile is characterized by overall intellectual disability, strength in concrete language, weakness in visuospatial construction, difficulties with sensory modulation, balance, and tool use, and problems with attention and anxiety. Structural and functional MRI studies demonstrate that gray matter deficiency in the intraparietal sulcus alters processing of spatial information in the dorsal stream (spatial) visual pathway, likely contributing to the visuospatial construction disability. Deficient regulation of the amygdala by the oribitofrontal cortex appears to underlie both the social disinhibition and the specific phobia common in WS. Continued study of cognition, behavior, neuroanatomy, and function in WS will continue to elucidate the neurogenetic underpinnings of human behavior.

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Section: Central Neurologic Signs and Neuroanatomymentioning

confidence: 99%

The behavioral phenotype of Williams syndrome: A recognizable pattern of neurodevelopment

Morris

2010

American J of Med Genetics Pt C

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“…Cherniske et al, 2004;Johnson et al, 2001;Marler et al, 2010). Hearing loss in WS subjects has, typically, early onset and is hypothesized to be progressive (Gothelf et al, 2006;Marler et al, 2005Marler et al, , 2010.…”

Section: Introductionmentioning

confidence: 99%

Cochlear active mechanisms in young normal-hearing subjects affected by Williams syndrome: Time–frequency analysis of otoacoustic emissions

et al. 2011

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“…[15][16][17][18] However, there is no evidence in our mice of a mechanism within the auditory signal processing pathway that might explain the auditory allodynia in WBS patients. 32 It is possible that this phenomenon results from Figure 5 Distortion products otoacoustic emission (DPOAE) thresholds.…”

Section: Discussionmentioning

confidence: 60%

“…[13][14][15] SNHL in WBS has been shown to be progressive and the prevalence may develop to~80% of subjects over time. 16 Although many younger WBS patients seem to have hearing in the normal range, it is generally agreed that analysis of otoacoustic emissions from the cochlea of these patients indicates high rates of abnormalities, [15][16][17][18] suggesting a degree of 'cochlear fragility', 15 associated with altered sound transduction. Measurement of the distortion product of otoacoustic emissions (DPOAEs) is a non-invasive, highly sensitive, objective measure of the cochlear amplifier mechanism mediated by the outer hair cells.…”

Section: Introductionmentioning

confidence: 99%

“…16 The cause of the auditory pathology in WBS is currently unknown and has led some to speculate on a possible contribution from the observed effects of premature ageing and/or a high predisposition for noise-induced cochlear damage that could be connected to the so-called hyperacusis. 17 Involvement of the haploinsufficiency of elastin due to hemizygous loss of the ELN gene is a popular hypothesis 15,17,18 because of its profound impact on other organ systems and expression of the gene in several key hearing structures. Loss of the LIMK1 gene has also been implicated as it encodes a kinase that regulates actin reorganisation and has a role in the control of outer hair cell motility.…”

Section: Introductionmentioning

confidence: 99%

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The role of GTF2IRD1 in the auditory pathology of Williams–Beuren Syndrome

et al. 2014

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Williams-Beuren Syndrome (WBS) is a rare genetic condition caused by a hemizygous deletion involving up to 28 genes within chromosome 7q11.23. Among the spectrum of physical and neurological defects in WBS, it is common to find a distinctive response to sound stimuli that includes extreme adverse reactions to loud, or sudden sounds and a fascination with certain sounds that may manifest as strengths in musical ability. However, hearing tests indicate that sensorineural hearing loss (SNHL) is frequently found in WBS patients. The functional and genetic basis of this unusual auditory phenotype is currently unknown. Here, we investigated the potential involvement of GTF2IRD1, a transcription factor encoded by a gene located within the WBS deletion that has been implicated as a contributor to the WBS assorted neurocognitive profile and craniofacial abnormalities. Using Gtf2ird1 knockout mice, we have analysed the expression of the gene in the inner ear and examined hearing capacity by evaluating the auditory brainstem response (ABR) and the distortion product of otoacoustic emissions (DPOAE). Our results show that Gtf2ird1 is expressed in a number of cell types within the cochlea, and Gtf2ird1 null mice showed higher auditory thresholds (hypoacusis) in both ABR and DPOAE hearing assessments. These data indicate that the principal hearing deficit in the mice can be traced to impairments in the amplification process mediated by the outer hair cells and suggests that similar mechanisms may underpin the SNHL experienced by WBS patients.

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Auditory function and hearing loss in children and adults with Williams syndrome: Cochlear impairment in individuals with otherwise normal hearing

Cited by 38 publications

References 91 publications

The behavioral phenotype of Williams syndrome: A recognizable pattern of neurodevelopment

The behavioral phenotype of Williams syndrome: A recognizable pattern of neurodevelopment

Cochlear active mechanisms in young normal-hearing subjects affected by Williams syndrome: Time–frequency analysis of otoacoustic emissions

The role of GTF2IRD1 in the auditory pathology of Williams–Beuren Syndrome

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