<i>DYRK1A</i> pathogenic variants in two patients with syndromic intellectual disability and a review of the literature

Meissner, Laura E.; Macnamara, Ellen; D’Souza, Precilla; Yang, John Jeongseok; Vézina, Gilbert; Ferreira, Carlos R.; Zein, Wadih M.; Tifft, Cynthia J.; Adams, David R.

doi:10.1002/mgg3.1544

Cited by 11 publications

(10 citation statements)

References 15 publications

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“…Few years after, the first frameshift variant was described in a patient with similar features (Courcet et al , 2012). The clinical spectrum associated with DYRK1A pathogenic variants ( MRD7 for Mental Retardation 7 in OMIM ) was further refined with the publication of additional patients, presenting suggestive facial dysmorphism, severe speech impairment and feeding difficulty, while epilepsy and prenatal microcephaly were not always present (Bronicki et al , 2015; Blackburn et al , 2019a; van Bon et al , 2011, 2016; O’Roak et al , 2012; Courcet et al , 2012; Okamoto et al , 2015; Iglesias et al , 2014; Ruaud et al , 2015; Ji et al , 2015; Rump et al , 2016; Luco et al , 2016; Murray et al , 2017; Evers et al , 2017; Lee et al , 2020a; Dang et al , 2018; Qiao et al , 2019; Ernst et al , 2020; Tran et al , 2020; Møller et al , 2008; Fujita et al , 2010; Oegema et al , 2010; Yamamoto et al , 2011; Valetto et al , 2012; Kim et al , 2017; Meissner et al , 2020; Matsumoto et al , 1997). Pathogenic variants were also identified in cohorts of individuals with ASD (O’Roak et al , 2012), but all have ID (Earl et al , 2017).…”

Section: Inotroductionmentioning

confidence: 99%

Integrative approach to interpret DYRK1A variants, leading to a frequent neurodevelopmental disorder

Courraud

Chater‐Diehl

Durand

et al. 2021

Preprint

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ABBSTRACTDYRK1A-related intellectual disability (ID) is among the most frequent monogenic form of ID. We refined the description of this disorder by reporting clinical and molecular data of forty individuals with ID harboring DYRK1A variants. We developed a combination of tools to interpret missense variants, which remains a major challenge in human genetics: i) a specific DYRK1A clinical score, ii) amino acid conservation data generated from one hundred of DYRK1A sequences across different taxa, iii) in vitro overexpression assays to study level, cellular localization, and kinase activity of DYRK1A mutant proteins, and iv) a specific blood DNA methylation signature. This integrative approach was successful to reclassify several variants as pathogenic. However, we questioned the involvement of some others, such as p.Thr588Asn, yet reported as pathogenic, and showed it does not cause obvious phenotype in mice, emphasizing the need to take care when interpreting variants, even those occurring de novo.

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Section: Inotroductionmentioning

confidence: 99%

Integrative approach to interpret DYRK1A variants, leading to a frequent neurodevelopmental disorder

Courraud

Chater‐Diehl

Durand

et al. 2021

Preprint

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“…MRD7 has facial features such as prominent ears, deep-set eyes, upslanted palpebral fissures, a short nose with a broad nasal tip, and retrognathia. Given that the reported prevalence of MRD7 is less than 1/1,000,000 [1,2], which is rare compared to 1:10,000 to 30,000 for CdLS [9], it is not easy for nonexpert clinicians to differentiate these syndromes based on facial dysmorphisms. Therefore, Face2Gene helped us introduce candidate diseases for the patient.…”

Section: Mrd7mentioning

confidence: 99%

“…The overexpression of DYRK1A produces intellectual disabilities in DS. Contrarily, haploinsufficiency of DYRK1A through a heterozygous chromosomal loss or intragenic variants causes MRD7 [ 7 , 8 ], suggesting that DYRK1A influences the cognitive function in a dose-dependent manner [ 2 ]. Herein, we report a case of MRD7 in whom Face2Gene introduced several genetic syndromes, including MRD7, as candidates.…”

Section: Introductionmentioning

confidence: 99%

“…Intellectual developmental disorder, autosomal dominant 7 (MRD7; OMIM 614104), also known as DYRK1A (haploinsufficiency) syndrome, is a rare autosomal dominant disease with a prevalence of less than 1/1,000,000 [1][2][3]. MRD7 is characterized by microcephaly, intellectual disability, speech delay, feeding difficulties, and distinct facial dysmorphisms, including prominent ears, deep-set eyes, mild upslanted palpebral fissures, a short nose with a broad nasal tip, and retrognathia [1,4,5].…”

Section: Introductionmentioning

confidence: 99%

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Whole-Exome Sequencing Identified a Novel DYRK1A Variant in a Patient With Intellectual Developmental Disorder, Autosomal Dominant 7

Obara

Abe

Toyoshima

2023

Cureus

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Intellectual developmental disorder, autosomal dominant 7 (MRD7; OMIM 614104) is a rare disease characterized by microcephaly, intellectual disability, speech delay, feeding difficulties, and facial dysmorphisms. This disorder is caused by pathogenic/likely pathogenic variants of the DYRK1A gene, which encodes dual-specificity tyrosine-phosphorylation-regulated kinase 1A. Here, we report a case of MRD7 that was diagnosed using Face2Gene and whole-exome sequencing (WES). A 22-year-old man presented with microcephaly, intellectual disability, slender body, long slender fingers, and facial dysmorphisms. He was previously diagnosed with Cornelia de Lange syndrome (CdLS) at four years of age. However, his CdLS clinical diagnostic score was low at 22 years of age. The Face2Gene application introduced several candidate diseases including MRD7. Finally, by utilizing WES and Sanger sequencing analysis of cloned cDNA, we identified a novel heterozygous duplication variant (c.848dup, p.(Asn283LysfsTer6)) in the DYRK1A gene, which introduces a premature stop codon. This report provides more information about the phenotypic spectrum of a young adult patient with MRD7. Face2Gene helped us introduce candidate diseases of the patient. Registering further genetically confirmed cases with MRD7 will improve the accuracy of the diagnostic recommendations in Face2Gene. Moreover, WES is a powerful tool for diagnosing rare genetic diseases, such as MRD7.

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“…DYRK1A is a gene located on the critical region of chromosome 21q22 ( 1 ). It codifies for a dual-specificity tyrosine kinase, enrolled in the phosphorylation of serine and threonine residues ( 2 , 3 ) and tyrosine residues in their own loop ( 3 ). This protein is expressed in numerous systems and its role is pivotal, especially for neuronal differentiation, neurogenesis, and neurodegeneration ( 2 ) through MAP kinase activation.…”

Section: Introductionmentioning

confidence: 99%

Case Report: Gut and spleen anomalies associated with DYRK1A syndrome

et al. 2023

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DYRK1A syndrome has been extensively studied primarily with regard to neurologic and other phenotypic features such as skeleton and craniofacial alterations. In the present paper, we aim to highlight unusual anomalies associated with a DYRK1A mutation: a 17-year-old female patient with language and cognitive delay, microcephaly, and an autistic disorder, who was operated upon for spleen torsion with anomalous gut fixation.

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DYRK1A pathogenic variants in two patients with syndromic intellectual disability and a review of the literature

Abstract: This is an open access article under the terms of the Creative Commons Attribution License, which permits use, distribution and reproduction in any medium, provided the original work is properly cited.

Cited by 11 publications

References 15 publications

Integrative approach to interpret DYRK1A variants, leading to a frequent neurodevelopmental disorder

Integrative approach to interpret DYRK1A variants, leading to a frequent neurodevelopmental disorder

Whole-Exome Sequencing Identified a Novel DYRK1A Variant in a Patient With Intellectual Developmental Disorder, Autosomal Dominant 7

Case Report: Gut and spleen anomalies associated with DYRK1A syndrome

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