Vestibular <scp>phenotype‐genotype</scp> correlation in a cohort of 90 patients with Usher syndrome

Wafa, Talah; Faridi, Rabia; King, Kelly A.; Zalewski, Christopher; Yousaf, Rizwan; Schultz, Julie M.; Morell, Robert J.; Muskett, Julie; Turriff, Amy; Tsilou, Ekaterini; Griffith, Andrew J.; Friedman, Thomas B.; Zein, Wadih M.; Brewer, Carmen C.

doi:10.1111/cge.13868

Cited by 24 publications

(33 citation statements)

References 42 publications

(54 reference statements)

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“…USH is considered a rare disease, because it has a low prevalence, which ranges from 3 to 6.2 per 100,000 people [1]. Even though a recent report has cast doubts about the vestibular phenotypic differences among the USH subtypes [2], this disease is traditionally classified into three different subtypes depending on the age of onset, severity and progression of the symptoms, and the presence or absence of vestibular dysfunction [3]. USH type 1 (USH1) is the most severe subtype and is characterized by a severe to profound prelingual SNHL, early RP onset and vestibular alterations.…”

Section: Introductionmentioning

confidence: 99%

Usher Syndrome: Genetics of a Human Ciliopathy

Fuster-García

García‐Bohórquez

Rodríguez-Muñoz

et al. 2021

IJMS

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Usher syndrome (USH) is an autosomal recessive syndromic ciliopathy characterized by sensorineural hearing loss, retinitis pigmentosa and, sometimes, vestibular dysfunction. There are three clinical types depending on the severity and age of onset of the symptoms; in addition, ten genes are reported to be causative of USH, and six more related to the disease. These genes encode proteins of a diverse nature, which interact and form a dynamic protein network called the “Usher interactome”. In the organ of Corti, the USH proteins are essential for the correct development and maintenance of the structure and cohesion of the stereocilia. In the retina, the USH protein network is principally located in the periciliary region of the photoreceptors, and plays an important role in the maintenance of the periciliary structure and the trafficking of molecules between the inner and the outer segments of photoreceptors. Even though some genes are clearly involved in the syndrome, others are controversial. Moreover, expression of some USH genes has been detected in other tissues, which could explain their involvement in additional mild comorbidities. In this paper, we review the genetics of Usher syndrome and the spectrum of mutations in USH genes. The aim is to identify possible mutation associations with the disease and provide an updated genotype–phenotype correlation.

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Section: Introductionmentioning

confidence: 99%

Usher Syndrome: Genetics of a Human Ciliopathy

Fuster-García

García‐Bohórquez

Rodríguez-Muñoz

et al. 2021

IJMS

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“…Exceptions are reported where the most of pathological variants are usually responsible for profound congenital hearing loss with the absence of vestibular function. RP is also severe and rapidly progressive, with early onset [ 56 , 57 ]. Bilateral cochlear implantations (CIs) have provided strong evidence of successful rehabilitation among USH, DFNB2, or DFNA11.…”

Section: Genetics Of Ushmentioning

confidence: 99%

Usher Syndrome

Castiglione

Möller

2022

Audiology Research

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Usher syndrome (USH) is the most common genetic condition responsible for combined loss of hearing and vision. Balance disorders and bilateral vestibular areflexia are also observed in some cases. The syndrome was first described by Albrecht von Graefe in 1858, but later named by Charles Usher, who presented a large number of cases with hearing loss and retinopathy in 1914. USH has been grouped into three main clinical types: 1, 2, and 3, which are caused by mutations in different genes and are further divided into different subtypes. To date, nine causative genes have been identified and confirmed as responsible for the syndrome when mutated: MYO7A, USH1C, CDH23, PCDH15, and USH1G (SANS) for Usher type 1; USH2A, ADGRV1, and WHRN for Usher type 2; CLRN1 for Usher type 3. USH is inherited in an autosomal recessive pattern. Digenic, bi-allelic, and polygenic forms have also been reported, in addition to dominant or nonsyndromic forms of genetic mutations. This narrative review reports the causative forms, diagnosis, prognosis, epidemiology, rehabilitation, research, and new treatments of USH.

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“…USH type III is characterized by progressive postlingual hearing loss, variable onset of RP, and variable vestibular response ( Keats and Corey, 1999 ; Kimberling et al., 2010 ; Mathur and Yang, 2015 ). Vestibular-function phenotype does not, however, map exactly to USH subtype ( Wafa et al., 2021 ). To date, 12 genes have been associated with USH.…”

Section: Introductionmentioning

confidence: 97%

“…USH type III genes are CLRN1 and HARS1 ( Mathur and Yang, 2015 ). The roles of 3 are disputed; CIB2 , PDZD7 , and HARS are thought to be very rare contributors to USH ( Booth et al., 2018 ; Wafa et al., 2021 ). USH2A is most often identified as mutated in USH type II patients (80%); but ADGRV1 mutation also causes USH type II.…”

Section: Introductionmentioning

confidence: 99%

Trigenic ADH5/ALDH2/ADGRV1 mutations in myelodysplasia with Usher syndrome

Kinoshita

Ando

Ishii

et al. 2021

Heliyon

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Trio-next generation sequencing is useful to identify undiagnosed inherited diseases. We have attended a patient with trigenic ADH5 / ALDH2 / ADGRV1 pathogenic variants, which caused two distinct diseases, myelodysplastic syndrome and Usher syndrome. Whole genome sequencing of peripheral blood from the patient and his parents were applied to identify disease-causing genes. Sanger sequencing was performed to validate the identified ADH5 / ALDH2 / ADGRV1 variants. Our results identified disease-associated variants in ADGRV1 (disease inheritance autosomal recessive) and in ADH5 (disease inheritance also autosomal recessive) and a variant in ALDH2 (disease inheritance autosomal dominant). Although the variants identified in ADH5 and ALDH2 have been reported, their co-existence in association with disease-causing variation in a third gene has not. They broaden the spectrum of ADGRV1 in Usher syndrome. Findings on next generation sequencing guided rapid and accurate diagnosis, resulting in patient-tailored therapeutic intervention.

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Vestibular phenotype‐genotype correlation in a cohort of 90 patients with Usher syndrome

Cited by 24 publications

References 42 publications

Usher Syndrome: Genetics of a Human Ciliopathy

Usher Syndrome: Genetics of a Human Ciliopathy

Usher Syndrome

Trigenic ADH5/ALDH2/ADGRV1 mutations in myelodysplasia with Usher syndrome

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