A novel variant in WNT5A responsible for Robinow syndrome in a male fetus with limb shortening and agenesis of the penis

BACKGROUND:Psychiatric syndromes have polymorphic symptomatology, and are known to be heritable. Psychiatric symptoms (and even syndromes) often occur as part of the clinical presentation in rare Mendelian syndromes. Clinical exome sequencing reports may help with refining diagnosis and influence treatment decisions, in addition to providing a window into the biology of brain and behaviour. We describe a clinical audit of 12 individuals who sought treatment at our hospital, and for whom targeted sequencing was ordered. Three cases are discussed in detail to demonstrate correlations between genotype and phenotype in the clinic.METHODS:Targeted Next-Generation Sequencing (NGS) was done using Clinical Exome Panel (TruSight One, Illumina) covering coding exons and flanking intronic sequences of 4811 genes associated with known inherited diseases. Variants detected were classified according to the American College for Medical Genetics (ACMG) recommendation for standards of interpretation and reporting of sequence variations.RESULTS:Ten out of twelve cases had at least one pathogenic variant. In one of these cases, we detected a known pathogenic variant in MAPT gene in a suspected FTD case, which helped us to confirm the diagnosis. In another case, we detected a novel variant predicted to be deleterious in NF1 gene. Identification of this mutation suggested a change in treatment for the patient, that was of benefit. The same patient also harboured a novel variant in the TRIO gene. This gene may be involved in biological processes that underlie the patient’s psychiatric illness.CONCLUSIONS:The cases discussed here exemplify different scenarios under which targeted exome sequencing can find meaningful application in the clinic: confirming diagnosis (MAPT variant), or modifying treatment (NF1). We suggest that clinical exome sequencing can be a helpful addition to a clinician’s toolkit when there are expediting factors to consider— such as early-onset, strong family history of mental illness, complex/atypical presentations and minor physical anomalies or neurocutaneous markers.

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Faculty Opinions recommendation of On the probability that a novel variant is a disease-causing mutation.

Faculty Opinions – Post-Publication Peer Review of the Biomedical Literature ◽

10.3410/f.1027063.329637 ◽

2005 ◽

Author(s):

Darryl Nishimura

Keyword(s):

Novel Variant

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A Novel Variant of the Minimizing Re-Transmissions Technique for Wired Networks

Contemporary Research Trend of IT Convergence Technology ◽

10.21742/asehl.2016.4.24 ◽

2016 ◽

Author(s):

Nguyen Xuan Tien ◽

◽

Semog Kim ◽

Jong Myung Rhee ◽

◽

...

Keyword(s):

Wired Networks ◽

Novel Variant

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A novel missense TGFBI variant p.(Ser591Phe) in a Finnish family with variant lattice corneal dystrophy

European Journal of Ophthalmology ◽

10.1177/1120672121997305 ◽

2021 ◽

pp. 112067212199730

Author(s):

Aino Maaria Jaakkola ◽

Petri J Järventausta ◽

Reetta-Stiina Järvinen ◽

Pauliina Repo ◽

Tero T Kivelä ◽

...

Keyword(s):

Transforming Growth Factor Beta ◽

Transforming Growth Factor ◽

Late Onset ◽

Family Members ◽

Anterior Segment ◽

Corneal Dystrophy ◽

Ophthalmological Examination ◽

Lattice Corneal Dystrophy ◽

Tgfbi Gene ◽

Novel Variant

Introduction: We describe the phenotype of a variant lattice corneal dystrophy (LCD) potentially caused by a novel variant c.1772C>T p.(Ser591Phe) in exon 13 of the transforming growth factor beta-induced (TGFBI) gene. Case report: The proband, a 71-year-old woman referred because of bilateral LCD, first seen at the age of 65 years, with recent progressive symptoms, underwent a clinical ophthalmological examination, anterior segment optical coherence tomography and confocal microscopy. Additionally, three siblings and three children were examined. The identified TGFBI variant was screened in six family members using Sanger sequencing. A corneal dystrophy gene screen was performed for the proband. Translucent subepithelial irregularities and central to midperipheral stubby branching corneal stromal lattice lines, asymmetric between the right and the left eye, were visible and resulted in mild deterioration of vision in one eye. Genetic testing revealed a novel variant c.1772C>T in TGFBI, leading to the amino acid change p.(Ser591Phe). One daughter carried the same variant but had only thick stromal nerve fibres at the age of 49 years. The other family members neither had corneal abnormalities nor carried the variant. No keratoplasty is yet planned for the proband. Conclusions: We classify the novel variant in TGFBI as possibly pathogenic, potentially causing the late-onset, asymmetric variant LCD. Our findings add to the growing number of TGFBI variants associated with a spectrum of phenotypes of variant LCD.

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Efficient Batch and Fixed-Bed Sequestration of a Basic Dye using a Novel Variant of Ordered Mesoporous Carbon as Adsorbent

Arabian Journal of Chemistry ◽

10.1016/j.arabjc.2021.103186 ◽

2021 ◽

pp. 103186

Author(s):

Asna Mariyam ◽

Jyoti Mittal ◽

Farzeen Sakina ◽

Richard T. Baker ◽

Ashok K. Sharma ◽

...

Keyword(s):

Mesoporous Carbon ◽

Fixed Bed ◽

Ordered Mesoporous Carbon ◽

Basic Dye ◽

Ordered Mesoporous ◽

Novel Variant

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Development of a Viral-Like Particle Candidate Vaccine Against Novel Variant Infectious Bursal Disease Virus

Vaccines ◽

10.3390/vaccines9020142 ◽

2021 ◽

Vol 9 (2) ◽

pp. 142

Author(s):

Yulong Wang ◽

Nan Jiang ◽

Linjin Fan ◽

Li Gao ◽

Kai Li ◽

...

Keyword(s):

Disease Virus ◽

Infectious Bursal Disease Virus ◽

Protective Efficacy ◽

Expression System ◽

Size Exclusion ◽

Candidate Vaccine ◽

Infectious Bursal Disease ◽

Immune Protection ◽

Bursal Disease ◽

Novel Variant

Infectious bursal disease (IBD), an immunosuppressive disease of young chickens, is caused by infectious bursal disease virus (IBDV). Novel variant IBDV (nVarIBDV), a virus that can evade immune protection against very virulent IBDV (vvIBDV), is becoming a threat to the poultry industry. Therefore, nVarIBDV-specific vaccine is much needed for nVarIBDV control. In this study, the VP2 protein of SHG19 (a representative strain of nVarIBDV) was successfully expressed using an Escherichia coli expression system and further purified via ammonium sulfate precipitation and size-exclusion chromatography. The purified protein SHG19-VP2-466 could self-assemble into 25-nm virus-like particle (VLP). Subsequently, the immunogenicity and protective effect of the SHG19-VLP vaccine were evaluated using animal experiments, which indicated that the SHG19-VLP vaccine elicited neutralization antibodies and provided 100% protection against the nVarIBDV. Furthermore, the protective efficacy of the SHG19-VLP vaccine against the vvIBDV was evaluated. Although the SHG19-VLP vaccine induced a comparatively lower vvIBDV-specific neutralization antibody titer, it provided good protection against the lethal vvIBDV. In summary, the SHG19-VLP candidate vaccine could provide complete immune protection against the homologous nVarIBDV as well as the heterologous vvIBDV. This study is of significance to the comprehensive prevention and control of the recent atypical IBD epidemic.

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Cobalamin J disease detected on newborn screening: Novel variant and normal neurodevelopmental course

American Journal of Medical Genetics Part A ◽

10.1002/ajmg.a.62170 ◽

2021 ◽

Author(s):

Nishitha R. Pillai ◽

Dana Miller ◽

Elizabeth I. Pierpont ◽

Susan A. Berry ◽

Anjali Aggarwal

Keyword(s):

Newborn Screening ◽

Novel Variant

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Transient neonatal diabetes due to a disease causing novel variant in the ATP-binding cassette subfamily C member 8 (ABCC8) gene unmasks maturity-onset diabetes of the young (MODY) diabetes cases within a family

Journal of Pediatric Endocrinology and Metabolism ◽

10.1515/jpem-2020-0462 ◽

2020 ◽

Vol 0 (0) ◽

Author(s):

Eleni Z Giannopoulou ◽

Olga Ovcarov ◽

Elisa De Franco ◽

Fabian Kassberger ◽

Susanne Nusser ◽

...

Keyword(s):

Autoimmune Diabetes ◽

Family Members ◽

Neonatal Diabetes ◽

Atp Binding ◽

Adult Onset ◽

Family History Of Diabetes ◽

Abcc8 Gene ◽

Onset Diabetes ◽

Novel Variant ◽

Atp Binding Cassette

AbstractObjectivesNeonatal diabetes mellitus (NDM) is a rare monogenic diabetes form, occurring mainly from ATP-binding cassette subfamily C member 8 (ABCC8) and KCNJ11 mutations. ABCC8 mutations have also been found to cause adult-onset diabetes. What is new?: •Novel ABCC8 mutation in an NDM case •Heterogeneous clinical presentation of diabetes and response to sulfonylurea therapy among family members with the same ABCC8 mutation.Case presentationWe report the case of a newborn with NDM and a heterozygous ABCC8 novel variant (c.3835G>A), successfully treated with sulfonylurea. The same ABCC8 variant was found in two other family members, already treated for type 2 diabetes.ConclusionsThis case demonstrates the variable phenotypic presentation of diabetes due to a novel ABCC8 mutation (c.3835G>A), ranging from transient NDM to adult-onset, insulin-demanding diabetes, among family members. Genetic testing in young individuals with a strong family history of diabetes, presenting with non-autoimmune diabetes is recommended as it can determine prognosis and treatment of affected family members.

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