Joubert syndrome: genotyping a Northern European patient cohort

Kroes, Hester Y.; Monroe, Glen R.; Zwaag, Bert van der; Duran, Karen; Kovel, Carolien G.F. de; Roosmalen, Mark J van; Harakaľová, Magdaléna; Nijman, Isaäc J; Kloosterman, Wigard P.; Giles, Rachel; Knoers, Nine V A M; Haaften, Gijs van

doi:10.1038/ejhg.2015.84

Cited by 61 publications

(69 citation statements)

References 38 publications

(47 reference statements)

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“…Mutations in more than 30 genes can cause JSRD phenotypes(Kroes et al, 2016; Suzuki et al, 2016), and at least 20 genes are associated with LCA(den Hollander, 2016; Jacobson et al, 2016). CEP290 mutations can result in multiple divergent phenotypes, including JSRD and LCA.…”

Section: Discussionmentioning

confidence: 99%

In Vitro Modeling Using Ciliopathy-Patient-Derived Cells Reveals Distinct Cilia Dysfunctions Caused by CEP290 Mutations

et al. 2017

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Summary Mutations in CEP290, a transition zone protein in primary cilia, cause diverse ciliopathies, including Leber congenital amaurosis (LCA) and Joubert syndrome related disorders (JSRD). We examined cilia biogenesis and function in cells derived from CEP290-LCA and CEP290-JSRD patients. CEP290 protein was reduced in LCA fibroblasts with no detectable impact on cilia; however, optic cups derived from iPSCs of CEP290-LCA patients displayed less-developed photoreceptor cilia. Lack of CEP290 in JSRD fibroblasts resulted in abnormal cilia and decreased ciliogenesis. We observed selectively reduced localization of ADCY3 and ARL13B. Notably, Hedgehog signaling was augmented in CEP290-JSRD because of enhanced ciliary transport of Smoothened and GPR161. These results demonstrate a direct correlation between the extent of ciliogenesis defect(s) in fibroblasts and photoreceptors with phenotypic severity in JSRD and LCA, respectively, and strengthen the role of CEP290 as a selective ciliary gatekeeper for transport of signaling molecules in and out of the cilium.

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Section: Discussionmentioning

confidence: 99%

In Vitro Modeling Using Ciliopathy-Patient-Derived Cells Reveals Distinct Cilia Dysfunctions Caused by CEP290 Mutations

et al. 2017

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“…Clinical diagnosis is often challenging, as some of the characteristic systemic features may not develop until later in infancy and adulthood or may even evolve and change over time. Several multigene panel approaches have been used for molecular characterization of specific retinal ciliopathies, such as BBS, Joubert syndrome, and Usher syndrome, yielding variable diagnostic rates 7,18,19,46,47 . Here, we first studied a more heterogeneous and large cohort of “non-naive”, i.e.…”

Section: Discussionmentioning

confidence: 99%

“…Next-generation sequencing (NGS) is a cost-effective approach for the genetic diagnosis of retinal diseases 16,17 . Several studies have focused on specific retinal ciliopathies, such as Bardet-Biedl syndrome (BBS) 18 and Joubert syndrome 7,19–21 , with a wide range of reported mutation detection rates depending on the number of targeted genes, NGS platform, and use of pre-screened or “naive” cases. In patients with complex atypical phenotypes, chromosomal microarray analysis may also be very useful for assessing contiguous gene deletion syndromes as a cause of disease co-occurrence 22 .…”

Section: Introductionmentioning

confidence: 99%

Combining targeted panel-based resequencing and copy-number variation analysis for the diagnosis of inherited syndromic retinopathies and associated ciliopathies

Sánchez‐Navarro

Silva

Blanco‐Kelly

et al. 2018

Sci Rep

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Inherited syndromic retinopathies are a highly heterogeneous group of diseases that involve retinal anomalies and systemic manifestations. They include retinal ciliopathies, other well-defined clinical syndromes presenting with retinal alterations and cases of non-specific multisystemic diseases. The heterogeneity of these conditions makes molecular and clinical characterization of patients challenging in daily clinical practice. We explored the capacity of targeted resequencing and copy-number variation analysis to improve diagnosis of a heterogeneous cohort of 47 patients mainly comprising atypical cases that did not clearly fit a specific clinical diagnosis. Thirty-three likely pathogenic variants were identified in 18 genes (ABCC6, ALMS1, BBS1, BBS2, BBS12, CEP41, CEP290, IFT172, IFT27, MKKS, MYO7A, OTX2, PDZD7, PEX1, RPGRIP1, USH2A, VPS13B, and WDPCP). Molecular findings and additional clinical reassessments made it possible to accurately characterize 14 probands (30% of the total). Notably, clinical refinement of complex phenotypes was achieved in 4 cases, including 2 de novo OTX2-related syndromes, a novel phenotypic association for the ciliary CEP41 gene, and the co-existence of biallelic USH2A variants and a Koolen-de-Vries syndrome–related 17q21.31 microdeletion. We demonstrate that combining next-generation sequencing and CNV analysis is a comprehensive and useful approach to unravel the extensive phenotypic and genotypic complexity of inherited syndromic retinopathies.

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“…There was only one carrier, a Central Asian individual, in the Greater Middle East Variome database. The p.Asn242Ser allele was previously reported in patients with JS from studying two large cohort [5][6][7] . The same homozygous mutation was also reported in a 21-year-old male diagnosed with COACH syndrome [9] .…”

Section: Genetic Studymentioning

confidence: 99%

“…TMEM67 is one of the most frequently mutated JS genes in patients from northern European and Japanese populations [5][6][7] . However, based on currently available data, it is not the common cause in the Middle Eastern and North African Arab populations [8] .…”

Section: Introductionmentioning

confidence: 99%

A Common Ancestral Asn242Ser Mutation in <b><i>TMEM67</i></b> Identified in Multiple Iranian Families with Joubert Syndrome

Dehghani

Mojarad²,

Karimiani³

et al. 2017

Public Health Genomics

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Background: Joubert syndrome (JS) is a clinically and genetically heterogeneous group of rare neurodevelopmental disorder characterised by peculiar midbrain-hindbrain malformation, known as the “molar tooth” sign. JS can manifest a broad range of signs and symptoms. The most common features of JS are hypotonia, ataxia, developmental delay/intellectual disability, abnormal eye movements, and neonatal breathing abnormalities. To date, 29 genes have been shown to cause JS. Methods: We employed whole-genome single nucleotide polymorphism genotyping in a group of Iranian families with JS and Sanger sequencing of a known mutation associated with JS located in a single homozygous regions shared by affected members of the families. Results: Homozygosity mapping uncovered a shared ∼2.2-Mb run of homozygosity on chromosome 8q21.3-q22.1 encompassing the known JS-causing TMEM67 gene. Sanger sequencing of a known mutation (NM_153704.5: c.725A>G; p.Asn242Ser) in TMEM67 identified from studying another Iranian family using whole-exome sequencing confirmed the presence of the homozygous mutation in 22 affected members of 12 nuclear families. “Molar tooth” sign of brain magnetic resonance imaging, moderate-to-severe neurodevelopmental delay, and abnormal eye movements were the most common features of affected individuals. In addition, liver disease, seizure, behavioural abnormalities, failure to thrive, and kidney disease were observed variably in some of the patients. Conclusion: We propose that Asn242Ser is a founder mutation in the Iranian population, which might explain a significant proportion of JS cases from eastern Iran. Therefore, screening for this variant should be considered for genetic testing in Iranian patients with JS. In addition, this finding is important for developing population-specific genetic testing in Iran.

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Joubert syndrome: genotyping a Northern European patient cohort

Cited by 61 publications

References 38 publications

In Vitro Modeling Using Ciliopathy-Patient-Derived Cells Reveals Distinct Cilia Dysfunctions Caused by CEP290 Mutations

In Vitro Modeling Using Ciliopathy-Patient-Derived Cells Reveals Distinct Cilia Dysfunctions Caused by CEP290 Mutations

Combining targeted panel-based resequencing and copy-number variation analysis for the diagnosis of inherited syndromic retinopathies and associated ciliopathies

A Common Ancestral Asn242Ser Mutation in <b><i>TMEM67</i></b> Identified in Multiple Iranian Families with Joubert Syndrome

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