Congenital cataract and macular hypoplasia in humans associated with a de novo mutation in CRYAA and compound heterozygous mutations in P

Abstract Background Spinal muscular atrophy (SMA) is a rare neuromuscular disorder threating hundreds of thousands of lives worldwide. And the severity of SMA differs among different clinical types, which has been demonstrated to be modified by factors like SMN2, SERF1, NAIP, GTF2H2 and PLS3. However, the severities of many SMA cases, especially the cases within a family, often failed to be explained by these modifiers. Therefore, other modifiers are still waiting to be explored. Case presentation In this study, we presented a rare case of SMA discordant family with a mild SMA male patient and a severe SMA female patient. The two SMA cases fulfilled the diagnostic criteria defined by the International SMA Consortium. With whole exome sequencing, we confirmed the heterozygous deletion of exon7 at SMN1 on the parents’ genomes and the homozygous deletions on the two patients’ genomes. The MLPA results confirmed the deletions and indicated that all the family members carry two copies of SMN2, SERF1, NAIP and GTF2H2. Further genomic analysis identified compound heterozygous mutations at TLL2 on the male patient’s genome, and compound heterozygous mutations at VPS13A and the de novo mutation at AGAP5 on female patient’s genome. TLL2 is an activator of myostatin, which negatively regulates the growth of skeletal muscle tissue. Mutation in TLL2 has been proved to increase muscular function in mice model. VPS13A encodes proteins that control the cycling of proteins through the trans-Golgi network to endosomes, lysosomes and the plasma membrane. And AGAP5 was reported to have GTPase activator activity. Conclusions We reported a case of SMA discordant family and identified mutations at TLL2, VPS13A and AGAP5 on the patients’ genomes. The mutations at TLL2 were predicted to be pathogenic and are likely to alleviate the severity of the male SMA patient. Our finding broadens the spectrum of genetic modifiers of SMA and will contribute to accurate counseling of SMA affected patients and families.

Download Full-text

Compound Heterozygous Mutations Including a De Novo Missense Mutation in ABCA12 Led to a Case of Harlequin Ichthyosis with Moderate Clinical Severity

Journal of Investigative Dermatology ◽

10.1038/sj.jid.5700295 ◽

2006 ◽

Vol 126 (7) ◽

pp. 1518-1523 ◽

Cited By ~ 36

Author(s):

Masashi Akiyama ◽

Kaori Sakai ◽

Yoriko Sugiyama-Nakagiri ◽

Yasuko Yamanaka ◽

James R. McMillan ◽

...

Keyword(s):

Missense Mutation ◽

De Novo ◽

Clinical Severity ◽

Compound Heterozygous ◽

Harlequin Ichthyosis ◽

Compound Heterozygous Mutations

Download Full-text

Bile salt export pump deficiency: A de novo mutation in a child compound heterozygous forABCB11. Laboratory investigation to study pathogenic role and transmission of two novelABCB11mutations

Hepatology Research ◽

10.1111/j.1872-034x.2012.01061.x ◽

2013 ◽

Vol 43 (3) ◽

pp. 315-319 ◽

Cited By ~ 5

Author(s):

Paola Francalanci ◽

Isabella Giovannoni ◽

Manila Candusso ◽

Emanuele Bellacchio ◽

Francesco Callea

Keyword(s):

Bile Salt ◽

Laboratory Investigation ◽

De Novo ◽

De Novo Mutation ◽

Compound Heterozygous ◽

Bile Salt Export Pump ◽

Pathogenic Role

Download Full-text

A case of Idiopathic Infantile Hypercalcaemia (IIH) persisting into adulthood, caused by compound heterozygous mutations of 1,25-dihydroxyvitamin D2 24-hydroxylase (CYP24A1)

Endocrine Abstracts ◽

10.1530/endoabs.55.p27 ◽

2018 ◽

Author(s):

Victoria Stokes ◽

Caroline M Gorvin ◽

Bahram Jafar-Mohammadi ◽

Fiona Ryan ◽

Rajesh V Thakker

Keyword(s):

Compound Heterozygous ◽

Compound Heterozygous Mutations ◽

Idiopathic Infantile Hypercalcaemia

Download Full-text

A Case of Nonbullous Congenital Ichthyosiform Erythroderma Caused by Compound Heterozygous Mutations in TGM1

Nishi Nihon Hifuka ◽

10.2336/nishinihonhifu.81.103 ◽

2019 ◽

Vol 81 (2) ◽

pp. 103-105

Author(s):

Hitomi MARUSHIMA ◽

Yuka MIYOSHI ◽

Akemi TAKEMOTO ◽

Junji NAKANO

Keyword(s):

Compound Heterozygous ◽

Compound Heterozygous Mutations ◽

Congenital Ichthyosiform Erythroderma

Download Full-text

PROTEIN KINASE C DELTA (PRKCD) COMPOUND HETEROZYGOUS MUTATIONS IN SIBLINGS WITH RECURRENT INFECTIONS AND AUTOIMMUNITY

10.26226/morressier.594a7d45d462b8028d8931f4 ◽

2017 ◽

Author(s):

Marion Roderick

Keyword(s):

Protein Kinase C ◽

Protein Kinase ◽

Compound Heterozygous ◽

Recurrent Infections ◽

Protein Kinase C Delta ◽

Kinase C ◽

Compound Heterozygous Mutations

Download Full-text

Direct Transmission of Within-Host Mycobacterium Tuberculosis Diversity to Secondary Cases Can Lead to Variable Between-Host Heterogeneity Without De Novo Mutation: A Genomic Investigation

SSRN Electronic Journal ◽

10.2139/ssrn.3384856 ◽

2019 ◽

Author(s):

Marie Séraphin ◽

Anders Norman ◽

Erik Michael Rasmussen ◽

Alexandra M. Gerace ◽

Calin Chiribau ◽

...

Keyword(s):

Mycobacterium Tuberculosis ◽

De Novo ◽

De Novo Mutation ◽

Direct Transmission ◽

Host Heterogeneity

Download Full-text

Primary Microcephaly With Anterior Predominant Pachygyria Caused by Novel Compound Heterozygous Mutations in ASPM

Pediatric Neurology ◽

10.1016/j.pediatrneurol.2015.01.019 ◽

2015 ◽

Vol 52 (5) ◽

pp. e7-e8 ◽

Cited By ~ 4

Author(s):

Kazuyuki Nakamura ◽

Takehiko Inui ◽

Fuyuki Miya ◽

Yonehiro Kanemura ◽

Nobuhiko Okamoto ◽

...

Keyword(s):

Compound Heterozygous ◽

Primary Microcephaly ◽

Compound Heterozygous Mutations

Download Full-text

Intranasal oxytocin administration ameliorates social behavioral deficits in a POGZWT/Q1038R mouse model of autism spectrum disorder

Molecular Brain ◽

10.1186/s13041-021-00769-8 ◽

2021 ◽

Vol 14 (1) ◽

Author(s):

Kohei Kitagawa ◽

Kensuke Matsumura ◽

Masayuki Baba ◽

Momoka Kondo ◽

Tomoya Takemoto ◽

...

Keyword(s):

Autism Spectrum Disorder ◽

Social Behavior ◽

Mouse Model ◽

Mouse Models ◽

De Novo ◽

Neurodevelopmental Disorder ◽

Autism Spectrum ◽

Spectrum Disorder ◽

De Novo Mutation ◽

Behavioral Deficits

AbstractAutism spectrum disorder (ASD) is a highly prevalent neurodevelopmental disorder characterized by core symptoms of impaired social behavior and communication. Recent studies have suggested that the oxytocin system, which regulates social behavior in mammals, is potentially involved in ASD. Mouse models of ASD provide a useful system for understanding the associations between an impaired oxytocin system and social behavior deficits. However, limited studies have shown the involvement of the oxytocin system in the behavioral phenotypes in mouse models of ASD. We have previously demonstrated that a mouse model that carries the ASD patient-derived de novo mutation in the pogo transposable element derived with zinc finger domain (POGZWT/Q1038R mice), showed ASD-like social behavioral deficits. Here, we have explored whether oxytocin (OXT) administration improves impaired social behavior in POGZWT/Q1038R mice and found that intranasal oxytocin administration effectively restored the impaired social behavior in POGZWT/Q1038R mice. We also found that the expression level of the oxytocin receptor gene (OXTR) was low in POGZWT/Q1038R mice. However, we did not detect significant changes in the number of OXT-expressing neurons between the paraventricular nucleus of POGZWT/Q1038R mice and that of WT mice. A chromatin immunoprecipitation assay revealed that POGZ binds to the promoter region of OXTR and is involved in the transcriptional regulation of OXTR. In summary, our study demonstrate that the pathogenic mutation in the POGZ, a high-confidence ASD gene, impairs the oxytocin system and social behavior in mice, providing insights into the development of oxytocin-based therapeutics for ASD.

Download Full-text

Molecular basis of ciliary defects caused by compound heterozygous IFT144/WDR19 mutations found in cranioectodermal dysplasia

Human Molecular Genetics ◽

10.1093/hmg/ddab034 ◽

2021 ◽

Author(s):

Yamato Ishida ◽

Takuya Kobayashi ◽

Shuhei Chiba ◽

Yohei Katoh ◽

Kazuhisa Nakayama

Keyword(s):

Protein Trafficking ◽

Primary Cilia ◽

Intraflagellar Transport ◽

Missense Variant ◽

Cellular Level ◽

Compound Heterozygous ◽

Hypomorphic Allele ◽

Genes Encoding ◽

Specific Proteins ◽

Compound Heterozygous Mutations

Abstract Primary cilia contain specific proteins to achieve their functions as cellular antennae. Ciliary protein trafficking is mediated by the intraflagellar transport (IFT) machinery containing the IFT-A and IFT-B complexes. Mutations in genes encoding the IFT-A subunits (IFT43, IFT121/WDR35, IFT122, IFT139/TTC21B, IFT140, and IFT144/WDR19) often result in skeletal ciliopathies, including cranioectodermal dysplasia (CED). We here characterized the molecular and cellular defects of CED caused by compound heterozygous mutations in IFT144 [the missense variant IFT144(L710S) and the nonsense variant IFT144(R1103*)]. These two variants were distinct with regard to their interactions with other IFT-A subunits and with the IFT-B complex. When exogenously expressed in IFT144-knockout (KO) cells, IFT144(L710S) as well as IFT144(WT) rescued both moderately compromised ciliogenesis and the abnormal localization of ciliary proteins. As the homozygous IFT144(L710S) mutation was found to cause autosomal recessive retinitis pigmentosa, IFT144(L710S) is likely to be hypomorphic at the cellular level. In striking contrast, the exogenous expression of IFT144(R1103*) in IFT144-KO cells exacerbated the ciliogenesis defects. The expression of IFT144(R1103*) together with IFT144(WT) restored the abnormal phenotypes of IFT144-KO cells. However, the coexpression of IFT144(R1103*) with the hypomorphic IFT144(L710S) variant in IFT144-KO cells, which mimics the genotype of compound heterozygous CED patients, resulted in severe ciliogenesis defects. Taken together, these observations demonstrate that compound heterozygous mutations in IFT144 cause severe ciliary defects via a complicated mechanism, where one allele can cause severe ciliary defects when combined with a hypomorphic allele.

Download Full-text