A novel mutation and variable phenotypic expression in a large consanguineous pedigree with Jalili syndrome

Rahimi-Aliabadi, Simin; Daftarian, Narsis; Ahmadieh, Hamid; Emamalizadeh, Babak; Jamshidi, Javad; Tafakhori, Abbas; Ghaedi, Hamid; Noroozi, Rezvan; Taghavi, Shaghyegh; Ahmadifard, Azadeh; Alehabib, Elham; Andarva, Monavvar; Shokraeian, Parasto; Atakhorrami, Minoo; Darvish, Hossein

doi:10.1038/eye.2016.137

Cited by 10 publications

(4 citation statements)

References 21 publications

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“…Refractive error was unavailable due to the opaque lens of the two patients in this study. In other literatures, mild to moderate hyperopia, and posterior capsular cataracts were common among JS patients (Rahimi-Aliabadi et al, 2016;Wawrocka et al, 2017). In addition, strabismus and keratoconus were reported in a few cases (Maia et al, 2018;Purwar et al, 2015).…”

Section: Discussionmentioning

confidence: 83%

Novel homozygous nonsynonymous variant of CNNM4 gene in a Chinese family with Jalili syndrome

Yan-feng

et al. 2022

Molec Gen & Gen Med

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Section: Discussionmentioning

confidence: 83%

Novel homozygous nonsynonymous variant of CNNM4 gene in a Chinese family with Jalili syndrome

Yan-feng

et al. 2022

Molec Gen & Gen Med

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“…CNNM4 mutations have revealed clinical consequences which are limited to retinal function in CRD and bio‐mineralization of teeth in AI (Parry et al, ). Twenty‐four CNNM4 mutations, including a single base insertion, base pair duplication, missense changes, large deletions, and termination mutations have been characterized in patients suffering from JS around the world (Abu‐Safieh et al, ; Coppieters et al, ; Doucette et al, ; Huang et al, ; Jaouad et al, ; Kiessling, Mitter, Mitter, Langmann, & Müller, ; Lopez Torres, Schorderet, Schorderet, Valmaggia, & Todorova, ; Luder et al, ; Maia et al, ; Polok et al, ; Prasad et al, ; Rahimi‐Aliabadi et al, ; Topçu et al, ; Wang et al, ; Wawrocka et al, ; Zobor et al, ). These mutations presumably influence the divalent metal transporter function of CNNM4 protein.…”

Section: Discussionmentioning

confidence: 99%

A novel pathogenic missense variant in CNNM4 underlying Jalili syndrome: Insights from molecular dynamics simulations

Parveen

Mirza

Vanmeert

et al. 2019

Molec Gen & Gen Med

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Background Jalili syndrome (JS) is a rare cone‐rod dystrophy (CRD) associated with amelogenesis imperfecta (AI). The first clinical presentation of JS patients was published in 1988 by Jalili and Smith. Pathogenic mutations in the Cyclin and CBS Domain Divalent Metal Cation Transport Mediator 4 (CNNM4) magnesium transporter protein have been reported as the leading cause of this anomaly. Methods In the present study, a clinical and genetic investigation was performed in a consanguineous family of Pakistani origin, showing characteristic features of JS. Sanger sequencing was successfully used to identify the causative variant in CNNM4. Molecular dynamics (MD) simulations were performed to study the effect of amino acid change over CNNM4 protein. Results Sequence analysis of CNNM4 revealed a novel missense variant (c.1220G>T, p.Arg407Leu) in exon‐1 encoding cystathionine‐β‐synthase (CBS) domain. To comprehend the mutational consequences in the structure, the mutant p.Arg407Leu was modeled together with a previously reported variant (c.1484C>T, p.Thr495Ile) in the same domain. Additionally, docking analysis deciphered the binding mode of the adenosine triphosphate (ATP) cofactor. Furthermore, 60ns MD simulations were carried out on wild type (p.Arg407/p.Thr495) and mutants (p.Arg407Leu/p.Thr495Ile) to understand the structural and energetic changes in protein structure and its dynamic behavior. An evident conformational shift of ATP in the binding site was observed in simulated mutants disrupting the native ATP‐binding mode. Conclusion The novel identified variant in CNNM4 is the first report from the Pakistani population. Overall, the study is valuable and may give a novel insight into metal transport in visual function and biomineralization.

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“…A total of twenty-four CNNM4 mutations have been documented to cause Jalili syndrome (OMIM # 217080), a rare condition consisting of cone-rod dystrophy and amelogenesis imperfecta (AI) (http://jalili.co/CNNM4/cnnm4_muts&stats.htm; Michaelides et al 2004; Parry et al 2009; Polok et al 2009; Jalili 2010; Zobor et al 2012; Abu-Safieh et al 2013; Doucette et al 2013; Luder et al 2013; Coppieters et al 2014; Gerth-Kahlert et al 2015; Wang et al 2015; Prasad et al 2016; Rahimi-Aliabadi et al 2016; Topcu et al 2016; Cherkaoui Jaouad et al 2017). While our initial evaluation of the present family did not identify the AI, reassessment uncovered the severe dental abnormalities that necessitated extraction of all teeth and the fitting of dentures in affected, but not in unaffected siblings or parents.…”

Section: Discussionmentioning

confidence: 99%

Identification of a mutation in CNNM4 by whole exome sequencing in an Amish family and functional link between CNNM4 and IQCB1

Zhang

et al. 2018

Mol Genet Genomics

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We investigated an Amish family in which three siblings presented with an early-onset childhood retinal dystrophy inherited in an autosomal recessive fashion. Genome-wide linkage analysis identified significant linkage to marker D2S2216 on 2q11 with a two-point LOD score of 1.95 and a multi-point LOD score of 3.76. Whole exome sequencing was then performed for the three affected individuals and identified a homozygous nonsense mutation (c.C1813T, p.R605X) in the cyclin and CBS domain divalent metal cation transport mediator 4 (CNNM4) gene located within the 2p14-2q14 Jalili syndrome locus. The initial assessment and collection of the family were performed before the clinical delineation of Jalili syndrome. Another assessment was made after the discovery of the responsible gene and the dental abnormalities characteristic of Jalili syndrome were retrospectively identified. The p.R605X mutation represents the first probable founder mutation of Jalili syndrome identified in the Amish community. The molecular mechanism underlying Jalili syndrome is unknown. Here we show that CNNM4 interacts with IQCB1, which causes Leber congenital amaurosis (LCA) when mutated. A truncated CNNM4 protein starting at R605 significantly increased the rate of apoptosis, and significantly increased the interaction between CNNM4 and IQCB1. Mutation p.R605X may cause Jalili syndrome by a nonsense-mediated decay mechanism, affecting the function of IQCB1 and apoptosis, or both. Our data, for the first time, functionally link Jalili syndrome gene CNNM4 to LCA gene IQCB1, providing important insights into the molecular pathogenic mechanism of retinal dystrophy in Jalili syndrome.

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A novel mutation and variable phenotypic expression in a large consanguineous pedigree with Jalili syndrome

Cited by 10 publications

References 21 publications

Novel homozygous nonsynonymous variant of CNNM4 gene in a Chinese family with Jalili syndrome

Novel homozygous nonsynonymous variant of CNNM4 gene in a Chinese family with Jalili syndrome

A novel pathogenic missense variant in CNNM4 underlying Jalili syndrome: Insights from molecular dynamics simulations

Identification of a mutation in CNNM4 by whole exome sequencing in an Amish family and functional link between CNNM4 and IQCB1

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