An Emerging Female Phenotype with Loss‐of‐Function Mutations in the
            <i>Aristaless‐</i>
            Related Homeodomain Transcription Factor
            <i>ARX</i>

Mattiske, Tessa; Moey, Ching; Vissers, Lisenka E L M; Thorne, Natalie; Georgeson, Peter; Bakshi, Madhura; Shoubridge, Cheryl

doi:10.1002/humu.23190

Cited by 13 publications

(13 citation statements)

References 27 publications

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“…The striking phenotypic differences between females with inherited X‐linked recessive ZC4H2 missense variants versus de novo X‐linked dominant deleterious ZC4H2 nonsense, frameshifting or Xq11.2 microdeletions is similar to that seen for a few other X‐linked genes, such as ARX (Bienvenu et al, ; Mattiske et al, ; Stromme et al, ), HDAC8 (Kaiser et al, ), PHF6 (Lower et al, ; Zweier et al, ), IQSEC2 (Ewans et al, ; O'Rawe et al, ; Shoubridge et al, ; Zerem et al, ), and CLCN4 (Hu et al, ; Palmer et al, ). Also gender‐specific pathogenicity differences of inherited variants in males and de novo variants in females have been reported for other XLID genes, for example, DDX3X (Dikow et al, ; Snijders Blok et al, ), KIAA2022 (Lorenzo et al, ; Van Maldergem et al, ), MTM1 (Schara, Kress, Tucke, & Mortier, ), and CASK (Moog et al, ).…”

Section: Discussionmentioning

confidence: 86%

Deleterious de novo variants of X‐linked ZC4H2 in females cause a variable phenotype with neurogenic arthrogryposis multiplex congenita

et al. 2019

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Pathogenic variants in the X-linked gene ZC4H2, which encodes a zinc-finger protein, cause an infrequently described syndromic form of arthrogryposis multiplex congenita (AMC) with central and peripheral nervous system involvement. We present genetic and detailed phenotypic information on 23 newly identified families and simplex cases that include 19 affected females from 18 families and 14 affected males from nine families. Of note, the 15 females with deleterious de novo ZC4H2 variants presented with phenotypes ranging from mild to severe, and their clinical features overlapped with those seen in affected males. By contrast, of the nine carrier females with inherited ZC4H2 missense variants that were deleterious in affected male relatives, four were symptomatic. We also compared clinical phenotypes with previously published cases of both sexes and provide an overview on 48 males and 57 females from 42 families. The spectrum of ZC4H2 defects comprises novel and recurrent mostly inherited missense variants in affected males, and de novo splicing, frameshift, nonsense, and partial ZC4H2 deletions in affected females. Pathogenicity of two newly identified missense variants was further supported by studies in zebrafish. We propose ZC4H2 as a good candidate for early genetic testing of males and females with a clinical suspicion of fetal hypo-/akinesia and/ or (neurogenic) AMC. K E Y W O R D S fetal hypo-/akinesia, club foot/-feet, complicated spastic paraplegia/ spasticity, Xq11.2 microdeletion, ZC4H2, ZC4H2-Associated Rare Disorders (ZARD) DDD study presents independent

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Section: Discussionmentioning

confidence: 86%

Deleterious de novo variants of X‐linked ZC4H2 in females cause a variable phenotype with neurogenic arthrogryposis multiplex congenita

et al. 2019

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“…A milder phenotype has been recently delineated in females with heterozygous XLAG mutations, with 31 affected carriers reported (Mattiske et al, 2017), which is additionally influenced by skewed X-inactivation, at least in brain (Marsh et al, 2009(Marsh et al, , 2016. Clinical manifestations mainly include ID and/or developmental delay (around half of the heterozygous female patients), partial or total ACC (around 73% of patients who underwent MRI), epilepsy (around 35%), and movement disorders (hypotonia/dystonia/ataxia, around 26%) (Mattiske et al, 2017). Behavioral disturbances and psychiatric features are also reported, such as autistic behavior, depression and anxiety.…”

Section: Discussionmentioning

confidence: 99%

Heterozygous nonsense ARX mutation in a family highlights the complexity of clinical and molecular diagnosis in case of chromosomal and single gene disorder co‐inheritance

Traversa

Marchionni

Giovannetti

et al. 2020

Molec Gen & Gen Med

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Background Corpus callosum agenesis (ACC) is one of the most frequent Central Nervous System (CNS) malformations. However, genetics underlying isolated forms is still poorly recognized. Here, we report on two female familial cases with partial ACC. The proband shows isolated partial ACC and a mild neurodevelopmental phenotype. A fetus from a previous interrupted pregnancy exhibited a complex phenotype including partial ACC and the occurrence of a de novo 17q12 microduplication, which was interpreted as probably disease‐causing. Methods A trio‐based clinical exome sequencing (CES) was performed. Results Clinical exome sequencing data analysis led to identifying a heterozygous nonsense variant (NM_139058.3:c.922G>T; NP_620689.1:p.Glu308Ter) in the aristaless related homeobox gene ( ARX ) in the proband, with a putative de novo occurrence, producing a hypothetical protein lacking two essential domains. Sanger analysis confirmed the wild‐type status of both parents in different tissues, and disclosed the occurrence of the nonsense variant in the fetus of the interrupted pregnancy, suggesting a formerly unrecognized contribution of the ARX mutation to the fetus' phenotype and gonadal or gonadosomatic mosaicism in one of the parents. Conclusion This study describes the phenotype associated with a heterozygous loss of function variant in ARX . Moreover, it highlights the importance of investigating both chromosomal and genetic contributions in cases of complex syndromic phenotypes involving CNS.

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“…As a consequence, heterozygous females typically have a milder disease phenotype or are not affected. Despite this, there is a growing list of X-chromosome genes which are subject to X-inactivation or escape X-inactivation, including, for example, PHF6, CLCN4, ALG13, ARX, or USP9X, DDX3X , which display distinct phenotypes in males and females depending on the functional severity of the variant, as well as manifesting in a more severe female phenotype than the heterozygous state would predict (4, 5, 6, 7, 8, 9, 10). We contend that the IQ motif and Sec7 domain 2 protein ( IQSEC2 ) (NM_001111125) (MIM 300522) is another X-chromosome disease gene in which we see a severe female phenotype because of heterozygous loss-of-function mutation.…”

Section: Introductionmentioning

confidence: 99%

Heterozygous loss of function of IQSEC2/Iqsec2 leads to increased activated Arf6 and severe neurocognitive seizure phenotype in females

et al. 2019

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Clinical presentations of mutations in the IQSEC2 gene on the X-chromosome initially implicated to cause non-syndromic intellectual disability (ID) in males have expanded to include early onset seizures in males as well as in females. The molecular pathogenesis is not well understood, nor the mechanisms driving disease expression in heterozygous females. Using a CRISPR/Cas9–edited Iqsec2 KO mouse model, we confirm the loss of Iqsec2 mRNA expression and lack of Iqsec2 protein within the brain of both founder and progeny mice. Both male (52%) and female (46%) Iqsec2 KO mice present with frequent and recurrent seizures. Focusing on Iqsec2 KO heterozygous female mice, we demonstrate increased hyperactivity, altered anxiety and fear responses, decreased social interactions, delayed learning capacity and decreased memory retention/novel recognition, recapitulating psychiatric issues, autistic-like features, and cognitive deficits present in female patients with loss-of-function IQSEC2 variants. Despite Iqsec2 normally acting to activate Arf6 substrate, we demonstrate that mice modelling the loss of Iqsec2 function present with increased levels of activated Arf6. We contend that loss of Iqsec2 function leads to altered regulation of activated Arf6-mediated responses to synaptic signalling and immature synaptic networks. We highlight the importance of IQSEC2 function for females by reporting a novel nonsense variant c.566C > A, p.(S189*) in an elderly female patient with profound intellectual disability, generalised seizures, and behavioural disturbances. Our human and mouse data reaffirm IQSEC2 as another disease gene with an unexpected X-chromosome heterozygous female phenotype. Our Iqsec2 mouse model recapitulates the phenotypes observed in human patients despite the differences in the IQSEC2/Iqsec2 gene X-chromosome inactivation between the species.

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An Emerging Female Phenotype with Loss‐of‐Function Mutations in the Aristaless‐ Related Homeodomain Transcription Factor ARX

Cited by 13 publications

References 27 publications

Deleterious de novo variants of X‐linked ZC4H2 in females cause a variable phenotype with neurogenic arthrogryposis multiplex congenita

Deleterious de novo variants of X‐linked ZC4H2 in females cause a variable phenotype with neurogenic arthrogryposis multiplex congenita

Heterozygous nonsense ARX mutation in a family highlights the complexity of clinical and molecular diagnosis in case of chromosomal and single gene disorder co‐inheritance

Heterozygous loss of function of IQSEC2/Iqsec2 leads to increased activated Arf6 and severe neurocognitive seizure phenotype in females

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