Your search keyword '"Dominant inheritance"' showing total 448 results

1. Prevalence and phenotypes associated with ALPK3 null variants in a large French multicentric cohort: Confirming its involvement in hypertrophic cardiomyopathy.

Author

Ader, Flavie, Jedraszak, Guillaume, Janin, Alexandre, Billon, Clarisse, Buisson, Nathalie Roux, Bloch, Adrien, Bensalah, Meriem, De Sandre‐Giovannoli, Anachiara, Goudal, Adeline, Marsili, Luisa, Cazeneuve, Cécile, Charron, Philippe, Millat, Gilles, and Richard, Pascale

Subjects

*HYPERTROPHIC cardiomyopathy, *NUCLEOTIDE sequencing, *CHILD patients, *GENETIC variation, *GENETIC testing, *EXOMES

Abstract

Biallelic disease‐causing variants in the ALPK3 gene were first identified in children presenting with a severe cardiomyopathy. More recently, it was shown that carriers of heterozygous ALPK3 null variants are at risk of developing hypertrophic cardiomyopathy (HCM) with an adult onset. Since the number of reported ALPK3 patients is small, the mutational spectrum and clinical data are not fully described. In this multi‐centric study, we described the molecular and clinical spectrum of a large cohort of ALPK3 patients. Genetic testing using targeted next generation sequencing was performed in 16 183 cardiomyopathy index cases. Thirty‐six patients carried at least one null ALPK3 variant. The five paediatric patients carried two ALPK3 variants, all presented an HCM phenotype with severe outcomes (one transplantation, one heart failure and one cardiac arrest). The 31 adult patients carried heterozygous variants and the main phenotype was HCM (n = 26/31); including 15% (n = 4) presented with an apical or a concentric form of hypertrophy. Reporting a large cohort of ALPK3 patients, this collaborative work confirmed a strong association with HCM and suggesting his screening in the context of idiopathic HCM. [ABSTRACT FROM AUTHOR]

Published

2024

2. A p.Val412Serfs pathogenic variant associated with Wolfram-like syndrome and leukodystrophy

Author

Ayca Kocaaga, Sevgi Yimenicioglu, and Murat Bayav

Subjects

Dominant inheritance, Leukodystrophy, Optic atrophy, WFS1 (Wolframin) gene, Wolfram-like syndrome, Neurosciences. Biological psychiatry. Neuropsychiatry, RC321-571

Abstract

Abstract Background Wolfram syndrome is due to a mutation of the WFS1 gene that codes for the transmembrane protein wolframin. This protein is located in the endoplasmic reticulum and is expressed at higher concentrations in the beta cells of pancreatic islets and the brain. The term "Wolfram syndrome spectrum" is often used because of its genetic and clinical heterogeneity. Disorders associated with the WFS1 gene include Wolfram syndrome following an autosomal recessive inheritance pattern and Wolfram-like syndrome following an autosomal dominant inheritance pattern, and congenital cataract. Here, we report a case with Wolfram-like syndrome presented with bilateral congenital cataract, optic atrophy, nystagmus, ataxia, mild intellectual disability, epilepsy and leukodystrophy. Case report Magnetic resonance imaging (MRI) showed bilateral cerebral T2 and flair hyperintensities that causes diffusion restriction in some areas with hypoperfusion. Bilateral T2 cerebellar central white matter hyperintensities and atrophy of brain stem were revealed by the brain MRI. There was also found evidence of a proximal cervical cord lesion and syrinx cavity in the vertebral MRI. The heterozygous frame-shift (c.1230_1233delCTCT; p.Val412Serfs) mutation in the WFS1 gene. This heterozygous pathogenic variant in the WFS1 gene was identified in both the father and grandmother. Conclusions To our knowledge, this is a novel Wolfram-like syndrome-related phenotype. This case report broadens the currently known phenotypic presentations of Wolfram-like syndrome and suggests that the p.Val412Serfs variant in the WFS1 gene may be associated with syrinx cavity and leukodystrophy.

Published

2023

3. A p.Val412Serfs pathogenic variant associated with Wolfram-like syndrome and leukodystrophy.

Author

Kocaaga, Ayca, Yimenicioglu, Sevgi, and Bayav, Murat

Subjects

*LEUKODYSTROPHY, *PANCREATIC beta cells, *CEREBRAL atrophy, *MAGNETIC resonance imaging, *GENETIC variation, *DISABILITIES

Abstract

Background: Wolfram syndrome is due to a mutation of the WFS1 gene that codes for the transmembrane protein wolframin. This protein is located in the endoplasmic reticulum and is expressed at higher concentrations in the beta cells of pancreatic islets and the brain. The term "Wolfram syndrome spectrum" is often used because of its genetic and clinical heterogeneity. Disorders associated with the WFS1 gene include Wolfram syndrome following an autosomal recessive inheritance pattern and Wolfram-like syndrome following an autosomal dominant inheritance pattern, and congenital cataract. Here, we report a case with Wolfram-like syndrome presented with bilateral congenital cataract, optic atrophy, nystagmus, ataxia, mild intellectual disability, epilepsy and leukodystrophy. Case report: Magnetic resonance imaging (MRI) showed bilateral cerebral T2 and flair hyperintensities that causes diffusion restriction in some areas with hypoperfusion. Bilateral T2 cerebellar central white matter hyperintensities and atrophy of brain stem were revealed by the brain MRI. There was also found evidence of a proximal cervical cord lesion and syrinx cavity in the vertebral MRI. The heterozygous frame-shift (c.1230_1233delCTCT; p.Val412Serfs) mutation in the WFS1 gene. This heterozygous pathogenic variant in the WFS1 gene was identified in both the father and grandmother. Conclusions: To our knowledge, this is a novel Wolfram-like syndrome-related phenotype. This case report broadens the currently known phenotypic presentations of Wolfram-like syndrome and suggests that the p.Val412Serfs variant in the WFS1 gene may be associated with syrinx cavity and leukodystrophy. [ABSTRACT FROM AUTHOR]

Published

2023

4. ITGB5 mutation discovered in a Chinese family with blepharophimosis-ptosis-epicanthus inversus syndrome

Author

Cheng Tianling, Yuan Xiaobin, Yuan Shaopeng, Zhu Jianying, Tang Shengjian, and Zhang Yujie

Subjects

bpes, itgb5, whole-exome sequencing, pathogenic genes, dominant inheritance, Biology (General), QH301-705.5

Abstract

Blepharophimosis-ptosis-epicanthus inversus syndrome (BPES) is a rare autosomal-dominant genetic disorder, and mutations in the forkhead box L2 (FOXL2) gene are one of the major genetic causes. As this study shows, there are many patients with BPES who do not have FOXL2 mutations, as the screening results in all family members were negative. Using whole-exome sequence analysis, we discovered another possible mutational cause of BPES in integrin subunit beta 5 (ITGB5). The ITGB5 mutation (c.608T>C, p.Ile203Thr) appears in the base sequence of all BPES+ patients in this family, and it appears to be a three-generation-inherited mutation. It can cause changes in base sequence and protein function, and there may be cosegregation of disease phenotypes. ITGB5 is located on the long arm of chromosome three (3q21.2) and is close to the known pathogenic gene FOXL2 (3q23). This study is the first to report ITGB5 mutations in BPES, and we speculate that it may be directly involved in the pathogenesis of BPES or indirectly through the regulation of FOXL2.

Published

2021

5. Dominantly inherited muscle disorders: understanding their complexity and exploring therapeutic approaches.

Author

Findlay AR

Subjects

Humans, Animals, Muscular Diseases genetics, Muscular Diseases therapy, Muscular Diseases pathology, Genes, Dominant, Mutation genetics

Abstract

Treatments for disabling and life-threatening hereditary muscle disorders are finally close to becoming a reality. Research has thus far focused primarily on recessive forms of muscle disease. The gene replacement strategies that are commonly employed for recessive, loss-of-function disorders are not readily translatable to most dominant myopathies owing to the presence of a normal chromosome in each nucleus, hindering the development of novel treatments for these dominant disorders. This is largely due to their complex, heterogeneous disease mechanisms that require unique therapeutic approaches. However, as viral and RNA interference-based therapies enter clinical use, key tools are now in place to develop treatments for dominantly inherited disorders of muscle. This article will review what is known about dominantly inherited disorders of muscle, specifically their genetic basis, how mutations lead to disease, and the pathomechanistic implications for therapeutic approaches., Competing Interests: Competing interests The author is a co-inventor on patent US12043832B2., (© 2024. Published by The Company of Biologists Ltd.)

Published

2024

6. Active site variants in STT3A cause a dominant type I congenital disorder of glycosylation with neuromusculoskeletal findings.

Author

Wilson, Matthew P., Garanto, Alejandro, Pinto e Vairo, Filippo, Ng, Bobby G., Ranatunga, Wasantha K., Ventouratou, Marina, Baerenfaenger, Melissa, Huijben, Karin, Thiel, Christian, Ashikov, Angel, Keldermans, Liesbeth, Souche, Erika, Vuillaumier-Barrot, Sandrine, Dupré, Thierry, Michelakakis, Helen, Fiumara, Agata, Pitt, James, White, Susan M., Lim, Sze Chern, and Gallacher, Lyndon

Subjects

*CONGENITAL disorders, *GLYCOSYLATION, *MISSENSE mutation, *MUSCLE tone, *GENETIC variation, *TRANSFERRIN

Abstract

Congenital disorders of glycosylation (CDGs) form a group of rare diseases characterized by hypoglycosylation. We here report the identification of 16 individuals from nine families who have either inherited or de novo heterozygous missense variants in STT3A, leading to an autosomal-dominant CDG. STT3A encodes the catalytic subunit of the STT3A-containing oligosaccharyltransferase (OST) complex, essential for protein N-glycosylation. Affected individuals presented with variable skeletal anomalies, short stature, macrocephaly, and dysmorphic features; half had intellectual disability. Additional features included increased muscle tone and muscle cramps. Modeling of the variants in the 3D structure of the OST complex indicated that all variants are located in the catalytic site of STT3A, suggesting a direct mechanistic link to the transfer of oligosaccharides onto nascent glycoproteins. Indeed, expression of STT3A at mRNA and steady-state protein level in fibroblasts was normal, while glycosylation was abnormal. In S. cerevisiae , expression of STT3 containing variants homologous to those in affected individuals induced defective glycosylation of carboxypeptidase Y in a wild-type yeast strain and expression of the same mutants in the STT3 hypomorphic stt3-7 yeast strain worsened the already observed glycosylation defect. These data support a dominant pathomechanism underlying the glycosylation defect. Recessive mutations in STT3A have previously been described to lead to a CDG. We present here a dominant form of STT3A-CDG that, because of the presence of abnormal transferrin glycoforms, is unusual among dominant type I CDGs. [ABSTRACT FROM AUTHOR]

Published

2021

7. Analysis of the dominant mutation N188T of human connexin46 (hCx46) using concatenation and molecular dynamics simulation

Author

Patrik Schadzek, Yannick Stahl, Matthias Preller, and Anaclet Ngezahayo

Subjects

cataract, concatenation, dominant inheritance, hCx46, hCx46N188T, molecular dynamics, Biology (General), QH301-705.5

Abstract

Connexins (Cx) are proteins that form cell‐to‐cell gap junction channels. A mutation at position 188 in the second extracellular loop (E2) domain of hCx46 has been linked to an autosomal dominant zonular pulverulent cataract. As it is dominantly inherited, it is possible that the mutant variant affects the co‐expressed wild‐type Cx and/or its interaction with other cellular components. Here, we proposed to use concatenated hCx46wt‐hCx46N188T and hCx46N188T‐hCx46wt to analyze how hCx46N188T affected co‐expressed hCx46wt to achieve a dominant inheritance. Heterodimer hCx46wt‐hCx46N188T formed fewer gap junction plaques compared to homodimer hCx46wt‐hCx46wt, while the hCx46N188T‐hCx46N188T homodimer formed almost no gap junction plaques. Dye uptake experiments showed that hemichannels of concatenated variants were similar to hemichannels of monomers. Molecular dynamics simulations revealed that for docking, the N188 of a protomer was engaged in hydrogen bonds (HBs) with R180, N189, and D191 of the counterpart protomer of the adjacent hemichannel. T188 suppressed the formation of HBs between protomers. Molecular dynamics simulations of an equimolar hCx46wt/hCx46N188T gap junction channel revealed a reduced number of HBs between protomers, suggesting reduction of gap junction channels between lens fibers co‐expressing the variants.

Published

2019

8. Dominant Inheritance

Author

Rodriguez-Murillo, Laura, Salem, Rany M., and Gellman, Marc D., editor

Published

2020

9. Multigenerational case examples of hypophosphatasia: Challenges in genetic counseling and disease management

Author

Erin Huggins, Ricardo Ong, Cheryl Rockman-Greenberg, Lauren Bailey Flueckinger, Kathryn M. Dahir, and Priya S. Kishnani

Subjects

Hypophosphatasia, Alkaline phosphatase, Family history, Genetic counseling, ALPL gene, Dominant inheritance, Medicine (General), R5-920, Biology (General), QH301-705.5

Abstract

Hypophosphatasia (HPP) is an inherited metabolic condition caused by pathogenic mutations in the ALPL gene. This leads to deficiency of tissue non-specific alkaline phosphatase (TNSALP), resulting in decreased mineralization of the bones and/or teeth and multi-systemic complications. Inheritance may be autosomal dominant or recessive, and the phenotypic spectrum, including age of onset, varies widely. We present four families demonstrating both modes of inheritance of HPP and phenotypic variability and discuss the resultant challenges in disease management, genetic counseling, and risk assessment. Failure to consider different modes of inheritance in a family with HPP may lead to an inaccurate risk assessment upon which medical and reproductive decisions may be made. We highlight the essential role of high-quality genetic counseling and meaningful biochemical and molecular testing strategies in the evaluation and management of families with HPP.

Published

2020

10. Ancestral Variations of the PCDHG Gene Cluster Predispose to Dyslexia in a Multiplex Family

Author

Teesta Naskar, Mohammed Faruq, Priyajit Banerjee, Massarat Khan, Rashi Midha, Renu Kumari, Subhashree Devasenapathy, Bharat Prajapati, Sanghamitra Sengupta, Deepti Jain, Mitali Mukerji, Nandini Chatterjee Singh, and Subrata Sinha

Subjects

Dyslexia, Protocadherin gamma, Ancestral variations, Neanderthal genome, Dominant inheritance, Trans-homophilic interaction, Neuronal connection, Medicine, Medicine (General), R5-920

Abstract

Dyslexia is a heritable neurodevelopmental disorder characterized by difficulties in reading and writing. In this study, we describe the identification of a set of 17 polymorphisms located across 1.9 Mb region on chromosome 5q31.3, encompassing genes of the PCDHG cluster, TAF7, PCDH1 and ARHGAP26, dominantly inherited with dyslexia in a multi-incident family. Strikingly, the non-risk form of seven variations of the PCDHG cluster, are preponderant in the human lineage, while risk alleles are ancestral and conserved across Neanderthals to non-human primates. Four of these seven ancestral variations (c.460A > C [p.Ile154Leu], c.541G > A [p.Ala181Thr], c.2036G > C [p.Arg679Pro] and c.2059A > G [p.Lys687Glu]) result in amino acid alterations. p.Ile154Leu and p.Ala181Thr are present at EC2: EC3 interacting interface of γA3-PCDH and γA4-PCDH respectively might affect trans-homophilic interaction and hence neuronal connectivity. p.Arg679Pro and p.Lys687Glu are present within the linker region connecting trans-membrane to extracellular domain. Sequence analysis indicated the importance of p.Ile154, p.Arg679 and p.Lys687 in maintaining class specificity. Thus the observed association of PCDHG genes encoding neural adhesion proteins reinforces the hypothesis of aberrant neuronal connectivity in the pathophysiology of dyslexia. Additionally, the striking conservation of the identified variants indicates a role of PCDHG in the evolution of highly specialized cognitive skills critical to reading.

Published

2018

11. A single c.1715G>C calpain 3 gene variant causes dominant calpainopathy with loss of calpain 3 expression and activity.

Author

Vissing, John, Dahlqvist, Julia R., Roudaut, Carinne, Poupiot, Jerome, Richard, Isabelle, Duno, Morten, and Krag, Thomas

Abstract

Recessively inherited limb girdle muscular dystrophy (LGMD) type 2A is the most common LGMD worldwide. Here, we report the first single missense variant in CAPN3 causing dominantly inherited calpainopathy. A 43‐year‐old proband, his father and two sons were heterozygous for a c.1715G>C p.(Arg572Pro) variant in CAPN3. Affected family members had at least three of the following; muscle pain, a LGMD2A pattern of muscle weakness and wasting, muscle fat replacement on magnetic resonance imaging, myopathic muscle biopsy, and elevated creatine kinase. Total calpain 3 protein expression was 4 ± 3% of normal. In vitro analysis of c.1715G>C and the previously described c.643_663del variant indicated that the mutant proteins lack autolytic and proteolytic activity and decrease the quantity of wild‐type CAPN3 protein. Our findings suggest that dominantly inherited calpainopathy is not unique to the previously reported c.643_663del mutation of CAPN3, and that dominantly inherited calpainopathy should be considered for other single variations in CAPN3. [ABSTRACT FROM AUTHOR]

Published

2020

12. A novel mutation in the LRSAM1 gene in a family with early onset autosomal dominant Charcot-Marie-Tooth type 2P.

Author

Milella G, Amati A, Lastella P, Zanfardino P, Petruzzella V, and Zoccolella S

Subjects

Humans, Mutation genetics, Phenotype, Ubiquitin-Protein Ligases genetics, Charcot-Marie-Tooth Disease genetics

Abstract

Charcot-Marie-Tooth disease type 2P (CMT2P; MIM #614436) is a specific type of axonal neuropathy caused by mutations in the LRSAM1 gene, which is a RING-type E3 ubiquitin ligase. CMT2P can be inherited in two ways: as an autosomal dominant or autosomal recessive trait. In this report, we describe the clinical characteristics of a family with axonal sensory-motor neuropathy caused by a new variant of the LSRAM1 gene, which is associated with early-onset autosomal dominant CMT2P., Competing Interests: Declaration of Competing Interest None of the authors has any conflict of interest to disclose., (Copyright © 2024 Elsevier B.V. All rights reserved.)

Published

2024

13. Hereditary primary lateral sclerosis and progressive nonfluent aphasia.

Author

Gazulla, José, Ferrer, Isidro, Izquierdo-Alvarez, Silvia, Alvarez, Sara, Sánchez-Alcudia, Rocío, Bestué-Cardiel, María, Seral, María, Benavente, Isabel, Sierra-Martínez, Esther, and Berciano, José

Subjects

*FAMILIAL spastic paraplegia, *AMYOTROPHIC lateral sclerosis, *PYRAMIDAL tract, *APHASIA, *SPINAL cord, *MOTOR neurons, *ARM

Abstract

Objective: To report a kindred with an association between hereditary primary lateral sclerosis (PLS) and progressive nonfluent aphasia. Patients and methods: Six members from a kindred with 15 affected individuals spanning three generations, suffered from spasticity without muscle atrophy or fasciculation, starting in the lower limbs and spreading to the upper limbs and bulbar musculature, followed by effortful speech, nonfluent language and dementia, in 5 deceased members. Disease onset was during the sixth decade of life, or later. Cerebellar ataxia was the inaugural manifestation in two patients, and parkinsonism, in another. Results: Neuropathological examination in two patients demonstrated degeneration of lateral corticospinal tracts in the spinal cord, without loss of spinal, brainstem, or cerebral motor neurons. Greater loss of corticospinal fibers at sacral and lumbar, rather than at cervical or medullary levels was demonstrated, supporting a central axonal dying-back pathogenic mechanism. Marked reduction of myelin and nerve fibers in the frontal lobes was also present. Argyrophilic grain disease and primary age-related tauopathy were found in one case each, and considered incidental findings. Genetic testing, including exome sequencing aimed at PLS, ataxia, hereditary spastic paraplegia, and frontotemporal lobe dementia, triplet-repeated primed polymerase chain reaction aimed at dominant spinocerebellar ataxias, and massive sequencing of the human genome, yielded negative results. Conclusion: A central distal axonopathy affecting the corticospinal tract, exerted a pathogenic role in the dominantly inherited PLS-progressive nonfluent aphasia association, described herein. Further molecular studies are needed to identify the causative mutation in this disease. [ABSTRACT FROM AUTHOR]

Published

2019

14. Analysis of the dominant mutation N188T of human connexin46 (hCx46) using concatenation and molecular dynamics simulation.

Author

Schadzek, Patrik, Stahl, Yannick, Preller, Matthias, and Ngezahayo, Anaclet

Subjects

MOLECULAR dynamics, HETERODIMERS, CELL anatomy, HYDROGEN bonding, CONNEXINS, MONOMERS

Abstract

Connexins (Cx) are proteins that form cell‐to‐cell gap junction channels. A mutation at position 188 in the second extracellular loop (E2) domain of hCx46 has been linked to an autosomal dominant zonular pulverulent cataract. As it is dominantly inherited, it is possible that the mutant variant affects the co‐expressed wild‐type Cx and/or its interaction with other cellular components. Here, we proposed to use concatenated hCx46wt‐hCx46N188T and hCx46N188T‐hCx46wt to analyze how hCx46N188T affected co‐expressed hCx46wt to achieve a dominant inheritance. Heterodimer hCx46wt‐hCx46N188T formed fewer gap junction plaques compared to homodimer hCx46wt‐hCx46wt, while the hCx46N188T‐hCx46N188T homodimer formed almost no gap junction plaques. Dye uptake experiments showed that hemichannels of concatenated variants were similar to hemichannels of monomers. Molecular dynamics simulations revealed that for docking, the N188 of a protomer was engaged in hydrogen bonds (HBs) with R180, N189, and D191 of the counterpart protomer of the adjacent hemichannel. T188 suppressed the formation of HBs between protomers. Molecular dynamics simulations of an equimolar hCx46wt/hCx46N188T gap junction channel revealed a reduced number of HBs between protomers, suggesting reduction of gap junction channels between lens fibers co‐expressing the variants. [ABSTRACT FROM AUTHOR]

Published

2019

15. Type 2N von Willebrand disease: Is it always a recessive trait?

Author

Woods, Adriana Inés, Rossetti, Liliana Carmen, Paiva, Juvenal, De Brasi, Carlos Daniel, Romero, María Lucila, Casinelli, María Marta, Blanco, Alicia Noemí, and Sánchez-Luceros, Analía

Subjects

*VON Willebrand disease, *VON Willebrand factor

Published

2021

16. Active site variants in STT3A cause a dominant type I congenital disorder of glycosylation with neuromusculoskeletal findings

Author

Rita Barone, Filippo Vairo, Bobby G. Ng, Jaak Jaeken, Gert Matthijs, James Pitt, Thierry Dupré, Lyndon Gallacher, Liesbeth Keldermans, Helen Michelakakis, Marina Ventouratou, Susan M. White, Sze Chern Lim, Melissa Baerenfaenger, Mirian C. H. Janssen, Angel Ashikov, Karin Huijben, Sandrine Vuillaumier-Barrot, Diana Ballhausen, Daisy Rymen, Agustí Rodríguez-Palmero, Blai Morales-Romero, Antonia Ribes, Peter Witters, Heidi Peters, Erika Souche, Eva Morava, Agata Fiumara, Pascale de Lonlay, Matthew P. Wilson, Dirk Lefeber, Wasantha Ranatunga, Alejandro Garanto, Hudson H. Freeze, Christian Thiel, BioAnalytical Chemistry, and AIMMS

Subjects

Male, Mutant, congenital disorders of glycosylation, chemistry.chemical_compound, 0302 clinical medicine, Catalytic Domain, Missense mutation, Musculoskeletal Diseases, Genetics (clinical), Genes, Dominant, chemistry.chemical_classification, Genetics, 0303 health sciences, Metabolic Disorders Radboud Institute for Molecular Life Sciences [Radboudumc 6], Middle Aged, Disorders of movement Donders Center for Medical Neuroscience [Radboudumc 3], Pedigree, Oligosaccharyltransferase complex, Child, Preschool, glycosylation, Female, Adult, Heterozygote, Glycosylation, Adolescent, Protein subunit, Biology, Article, 03 medical and health sciences, All institutes and research themes of the Radboud University Medical Center, oligosaccharyltransferase complex, medicine, Humans, dominant inheritance, Amino Acid Sequence, 030304 developmental biology, Sequence Homology, Amino Acid, Oligosaccharyltransferase, Membrane Proteins, medicine.disease, chemistry, Hexosyltransferases, Nervous System Diseases, Glycoprotein, Congenital disorder of glycosylation, 030217 neurology & neurosurgery

Abstract

Congenital disorders of glycosylation (CDGs) form a group of rare diseases characterized by hypoglycosylation. We here report the identification of 16 individuals from nine families who have either inherited or de novo heterozygous missense variants in STT3A, leading to an autosomal-dominant CDG. STT3A encodes the catalytic subunit of the STT3A-containing oligosaccharyltransferase (OST) complex, essential for protein N-glycosylation. Affected individuals presented with variable skeletal anomalies, short stature, macrocephaly, and dysmorphic features; half had intellectual disability. Additional features included increased muscle tone and muscle cramps. Modeling of the variants in the 3D structure of the OST complex indicated that all variants are located in the catalytic site of STT3A, suggesting a direct mechanistic link to the transfer of oligosaccharides onto nascent glycoproteins. Indeed, expression of STT3A at mRNA and steady-state protein level in fibroblasts was normal, while glycosylation was abnormal. In S. cerevisiae, expression of STT3 containing variants homologous to those in affected individuals induced defective glycosylation of carboxypeptidase Y in a wild-type yeast strain and expression of the same mutants in the STT3 hypomorphic stt3-7 yeast strain worsened the already observed glycosylation defect. These data support a dominant pathomechanism underlying the glycosylation defect. Recessive mutations in STT3A have previously been described to lead to a CDG. We present here a dominant form of STT3A-CDG that, because of the presence of abnormal transferrin glycoforms, is unusual among dominant type I CDGs. ispartof: AMERICAN JOURNAL OF HUMAN GENETICS vol:108 issue:11 pages:2130-2144 ispartof: location:United States status: published

Published

2021

17. Genetic analysis of adults heterozygous for ALPL mutations.

Author

Taillandier, Agnès, Domingues, Christelle, Dufour, Annika, Debiais, Françoise, Guggenbuhl, Pascal, Roux, Christian, Cormier, Catherine, Cortet, Bernard, Porquet-Bordes, Valérie, Coury, Fabienne, Geneviève, David, Chiesa, Jean, Colin, Thierry, Fletcher, Elaine, Guichet, Agnès, Javier, Rose-Marie, Laroche, Michel, Laurent, Michael, Lausch, Ekkehart, and LeHeup, Bruno

Subjects

*HYPOPHOSPHATASIA, *BONE diseases, *JOINT pain, *GENETIC mutation, *GENETICS

Abstract

Hypophosphatasia (HPP) is a rare inherited metabolic bone disease due to a deficiency of the tissue nonspecific alkaline phosphatase isoenzyme (TNSALP) encoded by the ALPL gene. Patients have consistently low serum alkaline phosphatase (AP), so that this parameter is a good hallmark of the disease. Adult HPP is heterogeneous, and some patients present only mild nonpathognomonic symptoms which are also common in the general population such as joint pain, osteomalacia and osteopenia, chondrocalcinosis, arthropathy and musculoskeletal pain. Adult HPP may be recessively or dominantly inherited; the latter case is assumed to be due to the dominant negative effect (DNE) of missense mutations derived from the functional homodimeric structure of TNSALP. However, there is no biological argument excluding the possibility of other causes of dominant HPP. Rheumatologists and endocrinologists are increasingly solicited for patients with low AP and nonpathognomonic symptoms of HPP. Many of these patients are heterozygous for an ALPL mutation and a challenging question is to determine if these symptoms, which are also common in the general population, are attributable to their heterozygous ALPL mutation or not. In an attempt to address this question, we reviewed a cohort of 61 adult patients heterozygous for an ALPL mutation. Mutations were distinguished according to their statistical likelihood to show a DNE. One-half of the patients carried mutations predicted with no DNE and were slightly less severely affected by the age of onset, serum AP activity and history of fractures. We hypothesized that these mutations result in another mechanism of dominance or are recessive alleles. To identify other genetic factors that could trigger the disease phenotype in heterozygotes for potential recessive mutations, we examined the next-generation sequencing results of 32 of these patients for a panel of 12 genes involved in the differential diagnosis of HPP or candidate modifier genes of HPP. The heterozygous genotype G/C of the COL1A2 coding SNP rs42524 c.1645C > G (p.Pro549Ala) was associated with the severity of the phenotype in patients carrying mutations with a DNE whereas the homozygous genotype G/G was over-represented in patients carrying mutations without a DNE, suggesting a possible role of this variant in the disease phenotype. These preliminary results support COL1A2 as a modifier gene of HPP and suggest that a significant proportion of adult heterozygotes for ALPL mutations may have unspecific symptoms not attributable to their heterozygosity. [ABSTRACT FROM AUTHOR]

Published

2018

18. Clinically variable nemaline myopathy in a three-generation family caused by mutation of the skeletal muscle alpha-actin gene.

Author

Lehtokari, Vilma-Lotta, Gardberg, Maria, Pelin, Katarina, and Wallgren-Pettersson, Carina

Subjects

*MYOTONIA atrophica, *GENETIC mutation, *ACTIN, *PROTEIN genetics, *NEMALINE myopathy, *CHILD patients, *DIAGNOSIS

Abstract

We present here a Finnish nemaline myopathy family with a dominant mutation in the skeletal muscle α-actin gene, p.(Glu85Lys), segregating in three generations. The index patient, a 5-year-old boy, had the typical form of nemaline myopathy with congenital muscle weakness and motor milestones delayed but reached, while his mother never had sought medical attention for her very mild muscle weakness, and his maternal grandmother had been misdiagnosed as having myotonic dystrophy. This illustrates the clinical variability in nemaline myopathy. [ABSTRACT FROM AUTHOR]

Published

2018

19. Genetic and Clinical Features of Familial Adenomatous Polyposis (FAP) and Attenuated FAP

Author

Risio, Mauro, Venesio, Tiziana, Delaini, Gian Gaetano, editor, Skřička, Tomáš, editor, and Colucci, Gianluca, editor

Published

2009

20. Seleção precoce para resistência à vassoura-de-bruxa do cacaueiro em novas combinações parentais

Author

José Luis Pires, Antônio Alves Pimenta, and Edna Dora Martins Newman Luz

Subjects

clone (Java method), genetic control, biology, Inoculation, Broom, Botany, Plant culture, Recurrent selection, Plant Science, biology.organism_classification, Moniliophthora perniciosa, SB1-1110, Horticulture, melhoramento de plantas, QK1-989, plant breeding, Theobroma cacao, Plant breeding, Dominant inheritance, Selection (genetic algorithm), controle genético

Abstract

Progenies from 69 crosses between parents obtained by recurrent selection for resistance and yield were inoculated with Moniliophthora perniciosa basidiospores. The symptoms were evaluated and compared with those in the equally inoculated progenies of Catongo, SIC 23 and SCA 6. Forty-three of the new progenies did not differ statistically from SCA 6, while 10 new progenies were statistically better than this control. The female parents that can be highlighted are (P4B x SCA 6), (MA 16 x SCA 6), (CEPEC 86 x SCA 6), and the EET 75 clone. The best male parents were (CAB 214), (CAB 208) and (P4B x OC 67), which did not differ from each other. This study proved the existence of gene combinations between fathers and mothers, the occurrence of additive effects and the dominant inheritance of these factors, which should allow the selection of clones with higher resistance levels and durability. RESUMO Progênies de 69 cruzamentos entre genitores obtidos por seleção recorrente para resistência e produtividade foram inoculadas com basidiósporos de Moniliophthora perniciosa. Os sintomas foram avaliados e comparados com aqueles nas progênies de Catongo, SIC 23 e SCA 6, igualmente inoculadas. Quarenta e três das novas progênies não diferiram estatisticamente de SCA 6, enquanto 10 novas progênies foram estatisticamente melhores do que esse controle. Os genitores femininos que podem ser destacados são (P4B x SCA 6), (MA 16 x SCA 6), (CEPEC 86 x SCA 6) e o clone EET 75. Os melhores genitores do sexo masculino foram (CAB 214), (CAB 208) e (P4B x OC 67), que não diferiram entre si. Este estudo comprovou a existência de combinações gênicas entre pais e mães, a ocorrência de efeitos aditivos e a dominância na herança desses fatores, o que deve permitir a seleção de clones com maiores níveis de resistência e durabilidade.

Published

2021

21. KCNC3R420H, a K+ channel mutation causative in spinocerebellar ataxia 13 displays aberrant intracellular trafficking

Author

Carolina Gallego-Iradi, Justin S. Bickford, Swati Khare, Alexis Hall, Jerelyn A. Nick, Donya Salmasinia, Kolja Wawrowsky, Serguei Bannykh, Duong P. Huynh, Diego E. Rincon-Limas, Stefan M. Pulst, Harry S. Nick, Pedro Fernandez-Funez, and Michael F. Waters

Subjects

Spinocerebellar ataxia, Dominant inheritance, SCA13, KCNC3, Voltage-gated potassium channel, Golgi, Neurosciences. Biological psychiatry. Neuropsychiatry, RC321-571

Abstract

Spinocerebellar ataxia 13 (SCA13) is an autosomal dominant disease resulting from mutations in KCNC3 (Kv3.3), a voltage-gated potassium channel. The KCNC3R420H mutation was first identified as causative for SCA13 in a four-generation Filipino kindred with over 20 affected individuals. Electrophysiological analyses in oocytes previously showed that this mutation did not lead to a functional channel and displayed a dominant negative phenotype. In an effort to identify the molecular basis of this allelic form of SCA13, we first determined that human KCNC3WT and KCNC3R420H display disparate post-translational modifications, and the mutant protein has reduced complex glycan adducts. Immunohistochemical analyses demonstrated that KCNC3R420H was not properly trafficking to the plasma membrane and surface biotinylation demonstrated that KCNC3R420H exhibited only 24% as much surface expression as KCNC3WT. KCNC3R420H trafficked through the ER but was retained in the Golgi. KCNC3R420H expression results in altered Golgi and cellular morphology. Electron microscopy of KCNC3R420H localization further supports retention in the Golgi. These results are specific to the KCNC3R420H allele and provide new insight into the molecular basis of disease manifestation in SCA13.

Published

2014

22. Charcot–Marie–Tooth disease type 2F associated with biallelic HSPB1 mutations

Author

Davide Pareyson, Stefania Corti, Franco Taroni, Dario Ronchi, Francesca Balistreri, Giulia Manenti, Nereo Bresolin, Chiara Pisciotta, Paola Saveri, Daniele Velardo, Megi Meneri, Elena Abati, Giacomo P. Comi, and Stefania Magri

Subjects

0301 basic medicine, Prioritization, animal structures, In silico, Neurosciences. Biological psychiatry. Neuropsychiatry, Disease, medicine.disease_cause, 03 medical and health sciences, Tooth disease, 0302 clinical medicine, Heat shock protein, Medicine, RC346-429, Gene, Genetics, Mutation, Case Study, business.industry, General Neuroscience, 030104 developmental biology, Neurology. Diseases of the nervous system, Neurology (clinical), Dominant inheritance, business, 030217 neurology & neurosurgery, RC321-571

Abstract

Objective This work aims to expand knowledge regarding the genetic spectrum of HSPB1‐related diseases. HSPB1 is a gene encoding heat shock protein 27, and mutations in HSPB1 have been identified as the cause of axonal Charcot–Marie–Tooth (CMT) disease type 2F and distal hereditary motor neuropathy (dHMN). Methods Two patients with axonal sensorimotor neuropathy underwent detailed clinical examinations, neurophysiological studies, and next‐generation sequencing with subsequent bioinformatic prioritization of genetic variants and in silico analysis of the likely causal mutation. Results The HSPB1 p.S135F and p.R136L mutations were identified in homozygosis in the two affected individuals. Both mutations affect the highly conserved alpha‐crystallin domain and have been previously described as the cause of severe CMT2F/dHMN, showing a strictly dominant inheritance pattern. Interpretation Thus, we report for the first time two cases of biallelic HSPB1 p.S135F and p.R136L mutations in two families.

Published

2021

23. Rare form of autosomal dominant familial Cornelia de Lange syndrome due to a novel duplication in SMC3.

Author

Infante, Elena, Alkorta‐Aranburu, Gorka, and El‐Gharbawy, Areeg

Subjects

*DE Lange's syndrome, *HUMAN abnormalities, *GENETIC testing, *GENETIC mutation, *PHENOTYPES

Abstract

Key Clinical Message Clinical features are variable in patients with Cornelia de Lange syndrome (CdLS). Milder forms exist with structural maintenance of chromosomes 3 (SMC3) mutations. Inherited milder forms of CdLS are uncommon and may be missed if genetic testing is limited to Nipped-B-like protein (NIPBL) and SMC1A. Parental studies should be pursued if there is a history of learning disabilities and/or dysmorphic features. [ABSTRACT FROM AUTHOR]

Published

2017

24. Autosomal dominant familial Mediterranean fever in Northern European Caucasians associated with deletion of p.M694 residue--a case series and genetic exploration.

Author

Rowczenio, Dorota M., Iancu, Daniela S., Trojer, Hadija, Gilbertson, Janet A., Gillmore, Julian D., Wechalekar, Ashutosh D., Tekman, Mehmet, Stanescu, Horia C., Kleta, Robert, Lane, Thirusha, Hawkins, Philip N., and Lachmann, Helen J.

Subjects

*FEVER, *COLCHICINE, *AMYLOIDOSIS, *GENES, *GENETIC disorders, *GENETIC techniques, *HISTOLOGICAL techniques, *IMMUNOHISTOCHEMISTRY, *INFLAMMATION, *GENETIC mutation, *RADIONUCLIDE imaging, *GENOTYPES, *SYMPTOMS, *GENETICS, *THERAPEUTICS

Abstract

Objective. This study was undertaken to characterize the phenotype and response to treatment in patients with autosomal dominant FMF caused by MEFV p.M694del mutation and to use haplotype reconstruction to investigate the possibility of common ancestry. Methods. MEFV gene was analysed in 3500 subjects with suspected FMF referred to a single UK centre between 2002 and 2014. Patients with p.M694del underwent additional screening of the SAA1 gene as well as haplotype reconstruction of the MEFV locus. Results. The p.M694del variant was identified in 21 patients, sharing an identical disease haplotype that appears to have arisen about 550 years ago. The SAA1.1 allele was found in four patients, including two with AA amyloidosis. The clinical features comprised typical FMF symptoms with median age at onset of 18 years; three patients presented with AA amyloidosis, of whom two had had symptoms of FMF in retrospect. Fifteen patients had received colchicine treatment, all with excellent responses. Conclusion. The p.M694del variant is associated with autosomal dominantly inherited FMF in Northern European Caucasians. Symptoms may develop later in life than in classical recessive FMF but are otherwise similar, as is the response to colchicine treatment. The 14% incidence of AA amyloidosis may reflect delay in diagnosis associated with extreme rarity of FMF in this population. The common haplotype suggests a single founder living in about 1460. [ABSTRACT FROM AUTHOR]

Published

2017

25. The diagnostic protocol for hereditary spherocytosis‐2021 update

Author

Faquan Lin, Lin Liao, and Yangyang Wu

Subjects

Microbiology (medical), Hemolytic anemia, Erythrocyte Indices, Pediatrics, medicine.medical_specialty, Anemia, Thalassemia, Clinical Biochemistry, Review Article, Spherocytosis, Hereditary, Hereditary spherocytosis, Diagnosis, Differential, Immunology and Allergy, Medicine, Humans, erythrocyte membrane protein, hereditary spherocytosis, Diagnostic Errors, Mean corpuscular volume, Genetic testing, diagnostic protocol, dominant inheritance, medicine.diagnostic_test, business.industry, Biochemistry (medical), Public Health, Environmental and Occupational Health, Hematology, medicine.disease, anemia, Medical Laboratory Technology, Glucosephosphate Dehydrogenase Deficiency, Mutation, Practice Guidelines as Topic, Eosine Yellowish-(YS), Anemia, Hemolytic, Autoimmune, Autoimmune hemolytic anemia, Differential diagnosis, business

Abstract

Background Hereditary spherocytosis (HS), a commonly encountered hereditary hemolytic disease, is mostly inherited in an autosomal dominant manner. The clinical manifestations in patients with HS show obvious heterogeneity. Moreover, the sensitivity or specificity of some HS diagnostic tests are not ideal and may easily result in misdiagnosis or missed diagnosis in some patients. The objective of this study was to propose a simple and practical diagnostic protocol, which can contribute to the diagnosis of HS and its differential diagnosis with different types of hemolytic anemia such as thalassemia (THAL), autoimmune hemolytic anemia (AIHA), and glucose‐6‐phosphate dehydrogenase (G6PD) deficiency, thus, to provide an alternative simple and reliable method for better clinical diagnosis of HS. Methods Through combing our research with existing experimental technologies and studies, we propose a simple and practical protocol for HS diagnosis, which will help clinicians to improve HS diagnosis. Results Compared with the existing HS diagnostic protocols, the HS diagnostic protocol we proposed is simpler. In this new protocol, some experimental tests with ideal diagnostic efficiency are added, such as mean reticulocyte volume (MRV), mean sphered cell volume (MSCV), mean corpuscular volume (MCV), in combination with the observation of clinical manifestations, family investigation, routine tests for hemolytic anemia, genetic testing, and other screening tests. Conclusion The HS diagnostic protocol we proposed could improve the clinical practice and efficiency of HS diagnosis., Hereditary spherocytosis (HS), a commonly encountered hereditary hemolytic disease, is mostly inherited in an autosomal‐dominant manner. The clinical manifestations in patients with HS show obvious heterogeneity. Moreover, the sensitivity or specificity of some HS diagnostic tests is not ideal and may easily result in misdiagnosis or missed diagnosis in some patients. Therefore, we propose a simple and practical protocol for HS diagnosis, helping clinicians to improve HS diagnosis.

Published

2021

26. A heterozygous 21-bp deletion in CAPN3 causes dominantly inherited limb girdle muscular dystrophy.

Author

Vissing, John, Barresi, Rita, Witting, Nanna, Van Ghelue, Marijke, Gammelgaard, Lise, Bindoff, Laurence A., Straub, Volker, Lochmüller, Hanns, Hudson, Judith, Wahl, Christoph M., Arnardottir, Snjolaug, Dahlbom, Kathe, Jonsrud, Christoffer, and Duno, Morten

Subjects

*MUSCULAR dystrophy, *RECESSIVE genes, *CALPAIN, *GENETIC mutation, *MUSCLE diseases, *GENEALOGY, *GENES, *GENETIC techniques, *MUSCLE proteins, *PROTEOLYTIC enzymes, *RESEARCH funding, *GENETIC carriers

Abstract

Limb girdle muscular dystrophy type 2A is the most common limb girdle muscular dystrophy form worldwide. Although strict recessive inheritance is assumed, patients carrying a single mutation in the calpain 3 gene (CAPN3) are reported. Such findings are commonly attributed to incomplete mutation screening. In this investigation, we report 37 individuals (age range: 21-85 years, 21 females and 16 males) from 10 families in whom only one mutation in CAPN3 could be identified; a 21-bp, in-frame deletion (c.643_663del21). This mutation co-segregated with evidence of muscle disease and autosomal dominant transmission in several generations. Evidence of muscle disease was indicated by muscle pain, muscle weakness and wasting, significant fat replacement of muscles on imaging, myopathic changes on muscle biopsy and loss of calpain 3 protein on western blotting. Thirty-one of 34 patients had elevated creatine kinase or myoglobin. Muscle weakness was generally milder than observed in limb girdle muscular dystrophy type 2A, but affected the same muscle groups (proximal leg, lumbar paraspinal and medial gastrocnemius muscles). In some cases, the weakness was severely disabling. The 21-bp deletion did not affect mRNA maturation. Calpain 3 expression in muscle, assessed by western blot, was below 15% of normal levels in the nine mutation carriers in whom this could be tested. Haplotype analysis in four families from three different countries suggests that the 21-bp deletion is a founder mutation. This study provides strong evidence that heterozygosity for the c.643_663del21 deletion in CAPN3 results in a dominantly inherited muscle disease. The normal expression of mutated mRNA and the severe loss of calpain 3 on western blotting, suggest a dominant negative effect with a loss-of-function mechanism affecting the calpain 3 homodimer. This renders patients deficient in calpain 3 as in limb girdle muscular dystrophy type 2A, albeit in a milder form in most cases. Based on findings in 10 families, our study indicates that a dominantly inherited pattern of calpainopathy exists, and should be considered in the diagnostic work-up and genetic counselling of patients with calpainopathy and single-allele aberrations in CAPN3. [ABSTRACT FROM AUTHOR]

Published

2016

27. A de novo mutation in KCNN3 associated with autosomal dominant idiopathic non-cirrhotic portal hypertension.

Author

Koot, Bart G.P., Alders, Marielle, Verheij, Joanne, Beuers, Ulrich, and Cobben, Jan M.

Subjects

*PORTAL hypertension, *CIRRHOSIS of the liver, *HISTOPATHOLOGY, *LIVER abnormalities, *FAMILIAL diseases

Abstract

Non-cirrhotic portal hypertension is characterized by histopathological abnormalities in the liver, mostly affecting small intrahepatic portal veins that cause portal hypertension in the absence of cirrhosis. It can be secondary to coagulation disorders or toxic agents. However, most cases are idiopathic non-cirrhotic portal hypertension (INCPH) and familial cases are rare. We report a family in which a father and three of his four children conceived with three different mothers are affected by INCPH. Whole exome and Sanger sequencing showed the father to have a de novo single nucleotide substitution c.1348G>C in the KCNN3 gene that was transmitted to all three of his affected offspring. The KCNN3 gene encodes small conductance calcium-activated potassium (SK) channel 3. SK channels are involved in the regulation of arterial and venous vascular tone by causing smooth muscle relaxation on activation. No data exist on the expression and function of SK channels in portal veins. The autosomal dominant inheritance in this unique pedigree and the single de novo mutation identified, strongly suggests that KCNN3 mutations have a pathogenetic role in INCPH. [ABSTRACT FROM AUTHOR]

Published

2016

28. A Mutant eIF4E Confers Resistance to Potato Virus Y Strains and is Inherited in a Dominant Manner in the Potato Varieties Atlantic and Russet Norkotah.

Author

Arcibal, Erica, Morey Gold, Kaitlin, Rakotondrafara, Aurélie, Flaherty, Stephanie, Jiang, Jiming, and Jahn, Molly

Subjects

*POTATO virus Y, *EUKARYOTIC cell genetics, *CULTIVARS, *POTATOES, *POTYVIRIDAE, *PATHOGENIC microorganisms

Abstract

Potato Virus Y (PVY) is one of the most important pathogens affecting potato production worldwide. Here we tested the efficacy of engineered resistance against PVY in two popular susceptible potato varieties, Russet Norkotah and Atlantic. This resistance is based on the expression of a modified potato eIF4E gene containing mutations homologous to those in the recessive resistant allelic variant found in pepper. The expression of this eIF4E variant conferred differential resistance responses against three prevalent PVY strains including PVY, PVY and PVY in the five tested transgenic lines. When resistance was established, the virus was not detectable in the inoculated leaves, the newly emerged leaves, nor in the sprouted tubers. Some strains were restrained to a low but detectable level in some of the potato lines. Crosses between transformed and wild type lines demonstrated that the engineered resistance gene was inherited in a dominant manner. [ABSTRACT FROM AUTHOR]

Published

2016

29. GDAP1 mutations in Italian axonal Charcot–Marie–Tooth patients: Phenotypic features and clinical course.

Author

Pezzini, I., Geroldi, A., Capponi, S., Gulli, R., Schenone, A., Grandis, M., Doria-Lamba, L., La Piana, C., Cremonte, M., Pisciotta, C., Nolano, M., Manganelli, F., Santoro, L., Mandich, P., and Bellone, E.

Subjects

*CHARCOT-Marie-Tooth disease, *GANGLIOSIDES, *GENETIC mutation, *AXONS, *NUCLEOTIDE sequencing, *DNA copy number variations, *PATIENTS

Abstract

Mutations in the ganglioside-induced differentiation associated-protein 1 ( GDAP1 ) gene have been associated with both autosomal recessive (AR) and dominant (AD) Charcot–Marie–Tooth (CMT) axonal neuropathy. The relative frequency of heterozygous, dominant mutations in Italian CMT is unknown. We investigated the frequency of dominant mutations in GDAP1 in a cohort of 109 axonal Italian patients by sequencing genomic DNA and search for copy number variations. We also explored correlations with clinical features. All cases had already been tested for variants in common axonal AD genes. Eight patients (7.3%) harbored five already reported heterozygous mutations in GDAP1 (p.Arg120Gly, p.Arg120Trp, p.His123Arg, p.Gln218Glu, p.Arg226Ser). Mutations had different penetrances in the families; the onset of symptoms is in the first decade and progression is slower than usually seen in GDAP1 -related AR-CMT. We show that the relative frequency of mutations in GDAP was slightly higher than those observed in MFN2 and MPZ (7.3% vs 6.3% and 5.0%). The relatively milder clinical features and the quite indolent course observed are relevant for prognostic assessment. On the basis of our experience and the data reported here, we suggest GDAP1 as the first gene that should be analysed in Italian patients affected by CMT2. [ABSTRACT FROM AUTHOR]

Published

2016

30. Variants in KIF1A gene in dominant and sporadic forms of hereditary spastic paraparesis.

Author

Citterio, Andrea, Arnoldi, Alessia, Panzeri, Elena, Merlini, Luciano, D'Angelo, Maria, Musumeci, Olimpia, Toscano, Antonio, Bondi, Alice, Martinuzzi, Andrea, Bresolin, Nereo, and Bassi, Maria

Subjects

*PARAPARESIS, *MOVEMENT disorders, *KINESIN, *NEURODEGENERATION, *GENETIC research

Abstract

KIF1A gene encodes the kinesin 1a protein, an axonal motor protein working in cargo transport along neurites. Variants in KIF1A were identified in different forms of neurodegenerative diseases with dominant and recessive inheritance. Homozygous recessive mutations were found in the hereditary sensory and autonomic neuropathy type 2, HSAN2 and in a recessive subtype of hereditary spastic paraparesis, SPG30. De novo heterozygous dominant variants were found both in a dominant form of SPG30 (AD-SPG30) with one single family reported and in patients with different forms of progressive neurodegenerative diseases. We report the results of a genetic screening of 192 HSP patients, with the identification of four heterozygous variants in KIF1A in four cases, two of whom with family history for the disease. Three of the four variants fall within the motor domain, a frequent target for variants related to the AD-SPG30 subtype. The fourth variant falls downstream the motor domain in a region lacking any functional domain. The KIF1A-related patients show clinical pictures overlapping the known AD-SPG30 phenotype including pure and complicated forms with few differences. Of note, one of the families, originating from the Sicily island, carries the same variant p.S69L detected in the first AD-SPG30 family of Finnish origin reported; differently from the first one, the latter family shows a wide intra-familial phenotype variability. Overall, these data reveal a very low frequency of the AD-SPG30 subtype while confirming the presence of amino acid residues in the motor domain representing preferential targets for mutations, thereby supporting their functional relevance in kinesin 1a activity. [ABSTRACT FROM AUTHOR]

Published

2015

31. Unilateral benign yellow dot maculopathy

Author

Netan Choudhry, André S. Pollmann, R. Rishi Gupta, Erin Demmings, and Amit V. Mishra

Subjects

Drusen, medicine.medical_specialty, medicine.diagnostic_test, business.industry, Case Report, RE1-994, medicine.disease, Yellow dots, Yellow dot, 03 medical and health sciences, Ophthalmology, 0302 clinical medicine, Optical coherence tomography, Maculopathy, 030221 ophthalmology & optometry, medicine, Dominant inheritance, business, 030217 neurology & neurosurgery

Abstract

Purpose To describe a unique case of unilateral benign yellow dot maculopathy. Observations A 25-year-man was evaluated after incidental finding of yellow dots in the right macula. Optical coherence tomography and electrophysiologic testing were unremarkable. The findings were in keeping with a diagnosis of benign yellow dot maculopathy. Conclusions and importance Benign yellow dot maculopathy is a recently described entity with either a sporadic or dominant inheritance pattern. This is the first known report of the characteristic findings of this phenotype presenting unilaterally.

Published

2021

32. Burosumab versus conventional therapy in children with X-linked hypophosphataemia: a randomised, active-controlled, open-label, phase 3 trial

Author

Hae Il Cheong, Meng Mao, Ola Nilsson, Alison Skrinar, Gary S. Gottesman, Wolfgang Högler, Javier San Martin, Hiroyuki Tanaka, Noriyuki Namba, Raja Padidela, Francis H. Glorieux, Michael P. Whyte, Koji Muroya, Craig F Munns, Chao-Yin Chen, Andrew Biggin, Erik A. Imel, Etienne Sochett, Leanne Ward, Anthony A. Portale, Jill H. Simmons, Farzana Perwad, and Pisit Pitukcheewanont

Subjects

Male, Fibroblast growth factor 23, medicine.medical_specialty, Rickets, 030204 cardiovascular system & hematology, Antibodies, Monoclonal, Humanized, Severity of Illness Index, Elevated serum, 03 medical and health sciences, Child Development, 0302 clinical medicine, Unknown Significance, Phase (matter), Internal medicine, Clinical endpoint, Humans, Immunologic Factors, Medicine, 030212 general & internal medicine, Child, business.industry, Therapy group, Antibodies, Monoclonal, Infant, General Medicine, medicine.disease, Body Height, Fibroblast Growth Factor-23, Treatment Outcome, Child, Preschool, Female, Familial Hypophosphatemic Rickets, Open label, Dominant inheritance, business

Abstract

X-linked hypophosphataemia in children is characterised by elevated serum concentrations of fibroblast growth factor 23 (FGF23), hypophosphataemia, rickets, lower extremity bowing, and growth impairment. We compared the efficacy and safety of continuing conventional therapy, consisting of oral phosphate and active vitamin D, versus switching to burosumab, a fully human monoclonal antibody against FGF23, in paediatric X-linked hypophosphataemia.In this randomised, active-controlled, open-label, phase 3 trial at 16 clinical sites, we enrolled children with X-linked hypophosphataemia aged 1-12 years. Key eligibility criteria were a total Thacher rickets severity score of at least 2·0, fasting serum phosphorus lower than 0·97 mmol/L (3·0 mg/dL), confirmed PHEX (phosphate-regulating endopeptidase homolog, X-linked) mutation or variant of unknown significance in the patient or a family member with appropriate X-linked dominant inheritance, and receipt of conventional therapy for at least 6 consecutive months for children younger than 3 years or at least 12 consecutive months for children older than 3 years. Eligible patients were randomly assigned (1:1) to receive either subcutaneous burosumab starting at 0·8 mg/kg every 2 weeks (burosumab group) or conventional therapy prescribed by investigators (conventional therapy group). Both interventions lasted 64 weeks. The primary endpoint was change in rickets severity at week 40, assessed by the Radiographic Global Impression of Change global score. All patients who received at least one dose of treatment were included in the primary and safety analyses. The trial is registered with ClinicalTrials.gov, number NCT02915705.Recruitment took place between Aug 3, 2016, and May 8, 2017. Of 122 patients assessed, 61 were enrolled. Of these, 32 (18 girls, 14 boys) were randomly assigned to continue receiving conventional therapy and 29 (16 girls, 13 boys) to receive burosumab. For the primary endpoint at week 40, patients in the burosumab group had significantly greater improvement in Radiographic Global Impression of Change global score than did patients in the conventional therapy group (least squares mean +1·9 [SE 0·1] with burosumab vs +0·8 [0·1] with conventional therapy; difference 1·1, 95% CI 0·8-1·5; p0·0001). Treatment-emergent adverse events considered possibly, probably, or definitely related to treatment by the investigator occurred more frequently with burosumab (17 [59%] of 29 patients in the burosumab group vs seven [22%] of 32 patients in the conventional therapy group). Three serious adverse events occurred in each group, all considered unrelated to treatment and resolved.Significantly greater clinical improvements were shown in rickets severity, growth, and biochemistries among children with X-linked hypophosphataemia treated with burosumab compared with those continuing conventional therapy.Ultragenyx Pharmaceutical and Kyowa Kirin International.

Published

2019

33. Dominant Inheritance

Author

Rodriguez-Murillo, Laura, Salem, Rany M., Gellman, Marc D., editor, and Turner, J. Rick, editor

Published

2013

34. Identification and fine mapping of alien fragments associated with enhanced grain weight from Agropyron cristatum chromosome 7P in common wheat backgrounds

Author

Xu Liu, Xiuquan Li, Sun Yangyang, Shenghui Zhou, Jinpeng Zhang, Yuqing Lu, Haiming Han, Weihua Liu, Lihui Li, Mingjie Lyu, and Xinming Yang

Subjects

Genetics, food and beverages, Chromosome, Chromosome Mapping, Chromosomal translocation, Locus (genetics), General Medicine, Biology, biology.organism_classification, Chromosomes, Plant, Translocation, Genetic, Agropyron cristatum, Grain weight, Plant Breeding, Seeds, Dominant inheritance, Common wheat, Agropyron, Edible Grain, Agronomy and Crop Science, Gene, Triticum, Biotechnology

Abstract

An enhanced grain weight locus from Agropyron cristatum chromosome 7P was verified in two wheat backgrounds, localized to the 7PS1-2 region. Novel translocation lines with this locus were evaluated. Agropyron cristatum is a wild relative of wheat that harbours elite genes for wheat improvement. The wheat-A. cristatum 7P disomic addition line II-5-1 exhibits high grain weight. Here, to dissect the genetic basis of grain weight contributed by A. cristatum chromosome 7P in wheat backgrounds, four segregated populations of the addition line were developed and evaluated in two wheat backgrounds. The results showed that A. cristatum chromosome 7P can stably and significantly increase the grain weight by approximately 2 g, mainly by increasing grain length at different grain weight levels of the wheat background. The locus for increased grain weight from chromosome 7P shows dominant inheritance independent of the wheat background. Moreover, two deletion lines and 23 translocation lines were identified by cytological methods and molecular markers, and an enlarged chromosome 7P bin map was constructed with 158 STS markers and 40 bin intervals. With the genetic populations of these deletion and translocation lines, the genetic locus of increased grain weight was narrowed down to bin 7PS1-2. Two translocation lines (7PT-A18 and 7PT-B4) with smaller 7P chromosomal segments exhibited an increase in grain weight, grain length and grain width simultaneously. These translocation lines carrying the 7PS1-2 chromosomal fragment will be valuable genetic resources for wheat grain weight improvement. Collectively, this study uncovers the grain weight locus from chromosome 7P and provides novel pre-breeding lines with enhanced grain weight.

Published

2021

35. Comment on: Bi-allelic variants in genes previously associated with dominant inheritance: CACNA1A, RET and SLC20A2

Author

Alisdair McNeill

Subjects

Genetics, Allele, Dominant inheritance, Biology, Gene, Genetics (clinical)

Published

2021

36. Psychosis and Catatonia in Fragile X Syndrome

Author

Silvina Tonarelli, Aayush Shah, Kendall R Dempsey, Karishma Palvadi, and Mitra Keshtkarjahromi

Subjects

medicine.medical_specialty, Psychosis, Catatonia, fragile x syndrome, child and adolescent psychiatry, 030204 cardiovascular system & hematology, New onset, 03 medical and health sciences, 0302 clinical medicine, intellectual developmental disorder (idd), psychiatric comorbidities, first episode psychosis, Child and adolescent psychiatry, medicine, Genetics, Psychiatry, business.industry, General Engineering, medicine.disease, Fragile X syndrome, Developmental disorder, attention deficit hyperactivity disorder (adhd), antipsychotics, Neurology, Autism spectrum disorder, Dominant inheritance, catatonia, business, 030217 neurology & neurosurgery

Abstract

Fragile X syndrome is an inherited disorder with an X-linked dominant inheritance pattern that is the most commonly inherited cause of intellectual developmental disorder and has a strong association with autism spectrum disorder. This report describes the case of an 18-year-old male with fragile X syndrome and multiple psychiatric comorbidities who presented with new onset psychosis and catatonia.

Published

2021

37. KCNC3R420H, a K+ channel mutation causative in spinocerebellar ataxia 13 displays aberrant intracellular trafficking.

Author

Gallego-Iradi, Carolina, Bickford, Justin S., Khare, Swati, Hall, Alexis, Nick, Jerelyn A., Salmasinia, Donya, Wawrowsky, Kolja, Bannykh, Serguei, Huynh, Duong P., Rincon-Limas, Diego E., Pulst, Stefan M., Nick, Harry S., Fernandez-Funez, Pedro, and Waters, Michael F.

Subjects

*SPINOCEREBELLAR ataxia, *ELECTROPHYSIOLOGY, *GENETIC mutation, *IMMUNOHISTOCHEMISTRY, *GENE expression, *POTASSIUM channels, *ELECTRON microscopy

Abstract

Spinocerebellar ataxia 13 (SCA13) is an autosomal dominant disease resulting from mutations in KCNC3 (Kv3.3), a voltage-gated potassium channel. The KCNC3 R420H mutation was first identified as causative for SCA13 in a four-generation Filipino kindred with over 20 affected individuals. Electrophysiological analyses in oocytes previously showed that this mutation did not lead to a functional channel and displayed a dominant negative phenotype. In an effort to identify the molecular basis of this allelic form of SCA13, we first determined that human KCNC3 WT and KCNC3 R420H display disparate post-translational modifications, and the mutant protein has reduced complex glycan adducts. Immunohistochemical analyses demonstrated that KCNC3 R420H was not properly trafficking to the plasma membrane and surface biotinylation demonstrated that KCNC3 R420H exhibited only 24% as much surface expression as KCNC3 WT . KCNC3 R420H trafficked through the ER but was retained in the Golgi. KCNC3 R420H expression results in altered Golgi and cellular morphology. Electron microscopy of KCNC3 R420H localization further supports retention in the Golgi. These results are specific to the KCNC3 R420H allele and provide new insight into the molecular basis of disease manifestation in SCA13. [ABSTRACT FROM AUTHOR]

Published

2014

38. Heterozygous intragenic deletions of FREM1 are not associated with trigonocephaly

Author

Denny Schanze, Sandra L. Marles, Trilochan Sahoo, Jing Liu, Karine Hovanes, Patrick Frosk, Aziz Mhanni, Albert E. Chudley, A. J. Dawson, Martin Zenker, and Cheryl R. Greenberg

Subjects

Male, Heterozygote, Trigonocephaly, Pathology and Forensic Medicine, Craniosynostosis, 03 medical and health sciences, Craniosynostoses, medicine, Missense mutation, Humans, Fraser syndrome, Genetics (clinical), Alleles, Genetic Association Studies, 030304 developmental biology, Sequence Deletion, Genetics, 0303 health sciences, Comparative Genomic Hybridization, business.industry, 030305 genetics & heredity, General Medicine, Receptors, Interleukin, medicine.disease, Penetrance, Phenotype, Pediatrics, Perinatology and Child Health, FRAS1, Female, Disease Susceptibility, Anatomy, Dominant inheritance, business

Abstract

Recessive mutations in FRAS1-related extracellular matrix 1 (FREM1) are associated with two rare genetic disorders, Manitoba-oculo-tricho-anal (MOTA) and bifid nose with or without anorectal and renal anomalies (BNAR). Fraser syndrome is a more severe disorder that shows phenotypic overlap with both MOTA and anorectal and renal anomalies and results from mutations in FRAS1, FREM2 and GRIP1. Heterozygous missense mutations in FREM1 were reported in association with isolated trigonocephaly with dominant inheritance and incomplete penetrance. Moreover, large deletions encompassing FREM1 have been reported in association with a syndromic form of trigonocephaly and were designated as trigonocephaly type 2. Trigonocephaly results from premature closure of the metopic suture and typically manifests as a form of nonsyndromic craniosynostosis. We report on 20 patients evaluated for developmental delay and without abnormal metopic suture. Chromosomal microarray analysis revealed heterozygous FREM1 deletions in 18 patients and in 4 phenotypically normal parents. Two patients were diagnosed with MOTA and had homozygous FREM1 deletions. Therefore, although our results are consistent with the previous reports of homozygous deletions causing MOTA, we report no association between heterozygous FREM1 deletions and trigonocephaly in this cohort.

Published

2020

39. Biallelic variants in genes previously associated with dominant inheritance: CACNA1A, RET and SLC20A2

Author

Maria Isabel Alvarez-Mora, C Palma Milla, Juan Francisco Quesada-Espinosa, Ana Arteche-López, I Gomez Manjón, I Hidalgo Mayoral, M T Sánchez Calvin, J M Lezana Rosales, Miguel A. Martín, M. Moreno-García, L I González Granado, A Juarez Rufián, R Pérez de la Fuente, O Sierra Tomillo, I J Posada Rodríguez, P Ramos Gómez, Alberto Blázquez, and M J Gómez Rodríguez

Subjects

Adult, Male, CACNA1A gene, Biology, Article, Recessive inheritance, Loss of Function Mutation, Genetics, Inheritance Patterns, Missense mutation, Humans, Gene, Genetics (clinical), Alleles, Genes, Dominant, Brain Diseases, Sodium-Phosphate Cotransporter Proteins, Type III, Proto-Oncogene Proteins c-ret, Comment, Inheritance (genetic algorithm), Infant, Newborn, Phenotype, Pedigree, Female, Calcium Channels, Dominant inheritance

Abstract

A subset of families with co-dominant or recessive inheritance has been described in several genes previously associated with dominant inheritance. Those recessive families displayed similar, more severe, or even completely different phenotypes to their dominant counterparts. We report the first patients harboring homozygous disease-related variants in three genes that were previously associated with dominant inheritance: a loss-of-function variant in the CACNA1A gene and two missense variants in the RET and SLC20A2 genes, respectively. All patients presented with a more severe clinical phenotype than the corresponding typical dominant form. We suggest that co-dominant or recessive inheritance for these three genes could explain the phenotypic differences from those documented in their cognate dominant phenotypes. Our results reinforce that geneticists should be aware of the possible different forms of inheritance in genes when WES variant interpretation is performed. We also evidence the need to refine phenotypes and inheritance patterns associated with genes in order to avoid failures during WES analysis and thus, raising the WES diagnostic capacity in the benefit of patients.

Published

2020

40. Prenatal array comparative genomic hybridization in a well-defined cohort of high-risk pregnancies. A 3-year implementation results in a public tertiary academic referral hospital

Author

Vedran Stefanovic, Tiina Alitalo, and Laura Maaria Emilia Tanner

Subjects

0301 basic medicine, Adult, medicine.medical_specialty, Referral, Noninvasive Prenatal Testing, Pregnancy, High-Risk, 030105 genetics & heredity, Cohort Studies, Tertiary Care Centers, 03 medical and health sciences, 0302 clinical medicine, Pregnancy, medicine, Humans, Copy-number variation, Sibling, Increased nuchal translucency, Genetics (clinical), Finland, Retrospective Studies, Fetus, Comparative Genomic Hybridization, 030219 obstetrics & reproductive medicine, Obstetrics, business.industry, Obstetrics and Gynecology, 3. Good health, Chorionic Villi Sampling, Cohort, Female, Dominant inheritance, business, Comparative genomic hybridization

Abstract

Objective To find out whether the diagnostic yield of prenatal array comparative genomic hybridization (aCGH) can be improved by targeting preselected high-risk pregnancies. Method All the in-house arrays ordered by the Fetomaternal Medical Center from February 2016 until December 2018 were retrospectively analyzed. The indications for array analysis included fetal structural abnormalities, increased nuchal translucency ≥3.5 mm and a chromosomal abnormality in a parent or a sibling. Common aneuploidies were excluded. Results Diagnostic yield was 15.1% in the entire patient cohort and as high as 20% in fetuses with multiple structural anomalies. The diagnostic yield was lowest in the group with isolated growth retardation. A total of 76 copy number variants (CNVs) were reported from a total of 65 samples, including 16 CNVs associated with a well-described microdeletion/microduplication syndrome, six autosomal trisomies in mosaic form, and three pathogenic single-gene deletions with dominant inheritance and 12 CNVs known to be risk factors for eg developmental delay. Conclusion The diagnostic yield of aCGH was higher than what has previously been reported in less defined patient cohorts. However, the number of CNVs with unclear correlation to the fetal ultrasound findings was still relatively high. The importance of adequate pre- and posttest counseling must therefore be emphasized.

Published

2020

41. A single c.1715G>C calpain 3 gene variant causes dominant calpainopathy with loss of calpain 3 expression and activity

Author

Thomas Krag, Carinne Roudaut, John Vissing, Julia R. Dahlqvist, Morten Duno, Isabelle Richard, Jerome Poupiot, University of Copenhagen = Københavns Universitet (KU), Approches génétiques intégrées et nouvelles thérapies pour les maladies rares (INTEGRARE), Université d'Évry-Val-d'Essonne (UEVE)-Institut National de la Santé et de la Recherche Médicale (INSERM)-Université Paris-Saclay-Généthon, University of Copenhagen = Københavns Universitet (UCPH), and Richard, Isabelle

Subjects

Adult, Male, Proband, [SDV.BIO]Life Sciences [q-bio]/Biotechnology, Adolescent, Muscle Proteins, calpain 3, [SDV.GEN.GH] Life Sciences [q-bio]/Genetics/Human genetics, [SDV.BBM.BM] Life Sciences [q-bio]/Biochemistry, Molecular Biology/Molecular biology, medicine.disease_cause, Young Adult, 03 medical and health sciences, Genetics, medicine, Humans, Missense mutation, Child, Genetics (clinical), limb girdle muscular dystrophy, Aged, 030304 developmental biology, 0303 health sciences, Mutation, Muscle biopsy, dominant inheritance, biology, medicine.diagnostic_test, Calpain, 030305 genetics & heredity, Muscle weakness, [SDV.BBM.BM]Life Sciences [q-bio]/Biochemistry, Molecular Biology/Molecular biology, Middle Aged, medicine.disease, Molecular biology, Pedigree, [SDV.BIO] Life Sciences [q-bio]/Biotechnology, calpainopathy, Muscular Dystrophies, Limb-Girdle, [SDV.GEN.GH]Life Sciences [q-bio]/Genetics/Human genetics, biology.protein, Creatine kinase, medicine.symptom, Limb-girdle muscular dystrophy

Abstract

Recessively inherited limb girdle muscular dystrophy (LGMD) type 2A is the most common LGMD worldwide. Here, we report the first single missense variant in CAPN3 causing dominantly inherited calpainopathy. A 43-year-old proband, his father and two sons were heterozygous for a c.1715G>C p.(Arg572Pro) variant in CAPN3. Affected family members had at least three of the following; muscle pain, a LGMD2A pattern of muscle weakness and wasting, muscle fat replacement on MRI, myopathic muscle biopsy, and elevated creatine kinase. Total calpain 3 protein expression was 4 ± 3% of normal. In vitro analysis of c.1715G>C and the previously described c.643_663del variant indicated that the mutant proteins lack autolytic and proteolytic activity and decrease the quantity of wild-type CAPN3 protein. Our findings suggest that dominantly inherited calpainopathy is not unique to the previously reported c.643_663del mutation of CAPN3, and that dominantly inherited calpainopathy should be considered for other single variations in CAPN3. This article is protected by copyright. All rights reserved.

Published

2020

42. Type 2N von Willebrand disease: Is it always a recessive trait?

Author

Adriana Ines Woods, Liliana Carmen Rossetti, Carlos Daniel de Brasi, María Marta Casinelli, Alicia N. Blanco, Juvenal Paiva, María Lucila Romero, and Analía Sánchez-Luceros

Subjects

Genetics, von Willebrand Diseases, Phenotype, business.industry, von Willebrand Factor, Von Willebrand disease, Medicine, Humans, Hematology, von Willebrand Disease, Type 2, Dominant inheritance, business, medicine.disease

Published

2020

43. Polimorfismos de los genes JAG1, MEF2C y BDNF asociados con la densidad mineral ósea en mujeres del norte de México

Author

Hilda Guadalupe Ávila-Rodríguez, Erik Ramírez-López, Zacarías Jiménez-Salas, Eduardo Campos-Góngora, Sandra Marlen González-Peña, and Rafael Velázquez-Cruz

Subjects

Bone mineral, medicine.medical_specialty, Osteoporosis, Single-nucleotide polymorphism, Biology, medicine.disease, General Biochemistry, Genetics and Molecular Biology, Endocrinology, Internal medicine, medicine, SNP, Dominant inheritance, Genotyping, rs6265, Genetic composition

Abstract

Introducción. La osteoporosis se caracteriza por una baja densidad mineral ósea; la composición genética es uno de los factores que más influyen en ella, pero hay pocos estudios de genes asociados con esta condición en la población mexicana.Objetivo. Investigar la posible asociación de ocho polimorfismos de un solo nucleótido (Single Nucleotide Polymorphism, SNP) de los genes JAG1, MEF2C y BDNF con la densidad mineral ósea en mujeres del norte de México.Materiales y métodos. Participaron 124 mujeres de 40 a 80 años, sin parentesco entre ellas. Su densidad mineral ósea se determinó mediante absorciometría dual de rayos X y la genotipificación se hizo utilizando discriminación alélica mediante PCR en tiempo real; se estudiaron cuatro de los SNP del gen JAG1 (rs6514116, rs2273061, rs2235811 y rs6040061), tres del MEF2C (rs1366594, rs12521522 y rs11951031) y uno del BDNF (rs6265). El análisis estadístico de los datos obtenidos se hizo por regresión lineal.Resultados. El SNP rs2235811 presentó asociación significativa con la densidad mineral ósea de todo el cuerpo bajo el modelo de herencia dominante (p=0,024) y, aunque los otros SNP no tuvieron relación significativa con esta densidad, en ninguno de los modelos de herencia estudiados, se observó una tendencia hacia esta asociación.Conclusión. Los resultados sugieren que el SNP rs2235811 del gen JAG1 podría contribuir a la variación en la densidad mineral ósea de las mujeres del norte de México.

Published

2018

44. Clinically variable nemaline myopathy in a three-generation family caused by mutation of the skeletal muscle alpha-actin gene

Author

Katarina Pelin, Vilma-Lotta Lehtokari, Maria Gardberg, Carina Wallgren-Pettersson, Department of Medical and Clinical Genetics, Medicum, Molecular and Integrative Biosciences Research Programme, Katarina Pelin / Principal Investigator, Genetics, Biosciences, and University of Helsinki

Subjects

Male, 0301 basic medicine, Pathology, medicine.medical_specialty, Three-generation family, Dominant inheritance, Clinical variability, Myopathies, Nemaline, medicine.disease_cause, Myotonic dystrophy, 03 medical and health sciences, 0302 clinical medicine, Nemaline myopathy, medicine, Humans, Muscle, Skeletal, Gene, Genetics (clinical), Mutation, business.industry, Skeletal muscle, Muscle weakness, ta3121, medicine.disease, Congenital myopathy, Actins, Skeletal muscle alpha-actin, Phenotype, 030104 developmental biology, medicine.anatomical_structure, CONGENITAL MYOPATHY, ACTA1 MUTATION, Neurology, Child, Preschool, Alpha-Actin, Pediatrics, Perinatology and Child Health, 3111 Biomedicine, Neurology (clinical), medicine.symptom, business, 030217 neurology & neurosurgery

Abstract

We present here a Finnish nemaline myopathy family with a dominant mutation in the skeletal muscle alpha-actin gene, p.(Glu85Lys), segregating in three generations. The index patient, a 5-year-old boy, had the typical form of nemaline myopathy with congenital muscle weakness and motor milestones delayed but reached, while his mother never had sought medical attention for her very mild muscle weakness, and his maternal grandmother had been misdiagnosed as having myotonic dystrophy. This illustrates the clinical variability in nemaline myopathy. (C) 2017 Elsevier B.V. All rights reserved.

Published

2018

45. Genetics of Hypophosphatasia.

Author

Mornet, Etienne

Subjects

*HYPOPHOSPHATASIA, *PHOSPHORUS metabolism disorders, *MISSENSE mutation, *MEDICAL genetics, *PHENOTYPES, *GENETICS

Abstract

Hypophosphatasia (HPP) results from mutations in the ALPL gene, mostly missense mutations. The gene is subject to a very high allelic heterogeneity, and some of these mutations have a dominant negative effect, two features that explain the most part of the clinical heterogeneity. Severe forms of the disease (perinatal and infantile) are inherited as an autosomal recessive trait. In the milder forms, autosomal recessive and autosomal dominant inheritance coexist. Experimental data show that there is a good correlation between the severity of the disease and in vitro alkaline phosphatase activity of the mutant protein. As a consequence of the existence of dominant mutations, moderate forms may be recessively or dominantly inherited and are expected more frequent than severe forms. The incidence of severe forms, inherited as a recessive trait, has been estimated at 1/300,000 in Europe. Genetic counseling is difficult in families where the mode of inheritance is unclear, or in prenatal context because of the prenatal benign form that may mimic severe perinatal HPP. During the ten last years, the mechanism of mineralization has been greatly deciphered, pointing out others gene that could modulate the HPP phenotype and explain particular cases where the phenotype does not correlate with the phenotype. [ABSTRACT FROM AUTHOR]

Published

2013

46. Familial episodic ataxia in lambs.

Author

Mayhew, IG, Jolly, RD, Burnham, D, Ridler, AL, Poff, GJ, and Blair, HT

Subjects

ATAXIA, LAMBS, COACH syndrome, MOVEMENT disorders, NEUROLOGICAL disorders

Abstract

HISTORY: A similar episodic neurological disorder occurred in new born lambs on two unrelated properties involving disparate breeds of sheep. Because of the number of lambs born, cross-breeding and the fact it occurred in some mating groups and not others, a dominant mode of inheritance was, initially and separately, suspected in each case. The sires of affected lambs were apparently normal. Whereas one was New Zealand Romney, the other was a composite breed with East Friesian genetics, but both rams originated from the same source property. To investigate the pathogenesis of the disorder these two rams were acquired and mated with unrelated sheep, under experimental conditions in a more controlled environment. CLINICAL FINDINGS: A proportion of lambs born to both sires exhibited a similar neurological disorder. Some lambs were noted to be abnormal at birth, both on home properties and in the experimental flock. They tended to adopt a head and neck extended posture and were slow to get to their feet and suckle when they then became more or less normal. When forced to move, they and other more robust lambs elicited an asymmetric gait, base-wide extensor hypertonia (hypometria) of thoracic limbs and flexor hypertonia (hypermetria) of pelvic limbs. In some there was nystagmus. After several metres of asymmetric ataxic gait they would fall to one side, sometimes adopting a sitting position. Recovery usually occurred in one to several minutes. As lambs aged, it became more difficult to elicit the episodes of dysfunction and by 6 months of age they appeared normal. DIAGNOSIS: The disorder was diagnosed as a dominant familial episodic cerebellovestibular ataxia inherited as a dominant trait, with incomplete penetration of observed clinical signs and variable expressivity. CLINICAL RELEVANCE: A proportion of affected lambs are likely to die in the neonatal period so the specific nature of the disorder may go unrecognised. Because of incomplete penetrance and varying expressivity, many of the lambs carrying this mutation will survive without showing clinical signs and may enter breeding flocks, where the disorder may be perpetuated and contribute to neonatal deaths. [ABSTRACT FROM PUBLISHER]

Published

2013

47. Value of bilateral breast cancer for identification of rare recessive at-risk alleles: evidence for the role of homozygous GEN1 c.2515_2519delAAGTT mutation.

Author

Kuligina, Ekatherina, Sokolenko, Anna, Mitiushkina, Nathalia, Abysheva, Svetlana, Preobrazhenskaya, Elena, Gorodnova, Tatiana, Yanus, Grigoriy, Togo, Alexandr, Cherdyntseva, Nadezhda, Bekhtereva, Svetlana, Dixon, J., Larionov, Alexey, Kuznetsov, Sergey, and Imyanitov, Evgeny

Abstract

Virtually all known tumor predisposing genes have been identified via the analysis of familial cancer cases. Here we argue that this approach is likely to miss recessively acting cancer genes and suggest the analysis of family history-negative patients with multiple primary malignancies for identifying homozygous at-risk genotypes. We performed calculations showing that the homozygous carriers of rare recessive cancer predisposing alleles are unlikely to report a family history of the disease. We further revealed that the c.2515_2519delAAGTT homozygous mutation in a Holliday junction resolvase, GEN1, was overrepresented in women with bilateral breast cancer (BC) as compared to healthy controls [11/360 (3.1 %) vs. 18/1305 (1.4 %); odds ratio (OR) = 2.25 (1.02-4.75); p = 0.031], although this trend was not maintained in unilateral BC patients [23/1851 (1.2 %)]. Noticeably, presence of biallelic c.2515_2519delAAGTT mutation was associated with the absence of BC in mother both in bilateral and unilateral BC cases [7/239 (3.0 %) vs. 0/41 (0 %) and 21/1,558 (1.3 %) vs. 0/215 (0 %), respectively; Mantel-Haenszel p = 0.041]. Thus, this study suggests that identification of dominant and recessive cancer predisposing genes may require distinct study groups. [ABSTRACT FROM AUTHOR]

Published

2013

48. Analysis of MLL2 gene in the first Brazilian family with Kabuki syndrome.

Author

Kokitsu-Nakata, Nancy Mizue, Petrin, Aline Lourenço, Heard, Jason Paul, Vendramini-Pittoli, Siulan, Henkle, Laura E, dos Santos, Daniela Vera Cruz, Murray, Jeffrey Clark, and Richieri-Costa, Antonio

Abstract

Most patients with Kabuki syndrome (KS) are the only person in their family with the condition. However, familial cases of KS have been described showing evidence that this syndrome can be inherited as a dominant trait with variable expressivity. We report on two related individuals with facial findings characteristic of KS. The proposita had arched eyebrows, long and upward slanting palpebral fissures, cleft lip and palate, retromicrognathia, brachydactyly of hands and feet, stubby fingers, nail hypoplasia, and prominent finger pads. Her mother had eyebrows with dispersed lateral half, long and upward slanting palpebral fissures, retrognathia, abnormal and posteriorly rotated ears, prominent finger pads, brachydactyly of feet, learning difficulties, and psychomotor development delay. DNA sequencing revealed a novel missense mutation in the MLL2 gene in both the proposita and her mother. The mutation (p.R5432Q) was found in the exon 51, within the SET domain of the gene, which confers methyltransferase activity on the protein. Therefore, the epigenetic and transcriptional regulatory properties of this protein may be altered and this suggests that the mutation is the cause of phenotype observed in both the patient and her mother. The clinical signs and the molecular evidence in this family further support the notion that KS is an autosomal dominant condition with variable expressivity. To our knowledge this is the first report of a Brazilian family with recurrence of this syndrome. © 2012 Wiley Periodicals, Inc. [ABSTRACT FROM AUTHOR]

Published

2012

49. La protoporphyrie érythropoïétique : une maladie, deux gènes et trois mécanismes moléculaires

Author

Schmitt, C., Ducamp, S., Gouya, L., Deybach, J.-C., and Puy, H.

Subjects

*GENETIC disorders, *PORPHYRIA, *PORPHYRINS, *BIOSYNTHESIS, *PHOTOSENSITIVITY disorders, *GENETIC mutation, *GENE frequency

Abstract

Abstract: Erythropoietic protoporphyria (EPP) is an inherited disorder of heme biosynthesis that results from an accumulation of protoporphyrin IX in erythroid cells, plasma, skin and liver. EPP leads to acute photosensitivity and, in about 2% of patients, liver disease. EPP is a complex syndrome in which two genes are independently involved: FECH and ALAS2. More than 96% of unrelated EPP patients have ferrochelatase (FECH) deficiency (MIM 177000). Four percent of them present with autosomal recessive inheritance with two mutated FECH alleles. In dominant cases (95%) the inheritance of a common hypomorphic IVS3-48C FECH allele trans to a deleterious FECH mutation reduces FECH activity below a critical threshold. The frequency of the IVS3-48C allele differs widely from the Japanese (45%), to Black West Africans (<1%) populations. These differences in the frequency of this single common SNP account for the prevalence of overt EPP in different countries and for the absence of EPP in Black Africans. The phylogenic origin of the IVS3-48C haplotypes strongly suggests that the IVS3-48C allele arose from a single recent mutational event that occurred 60Kyears ago. Acquired somatic mutation of FECH secondary to myeloid disease may also exceptionally cause EPP (<1%). Finally, about 4% of unrelated EPP patients have X-linked dominant protoporphyria (XLDPP) (MIM 300752) caused by gain-of-function mutations in the ALAS2 gene leading to an increased erythroid heme biosynthesis and subsequently an accumulation of protoporphyrin without any FECH deficiency. [ABSTRACT FROM AUTHOR]

Published

2010

50. Characterization and bulk segregant analysis of ‘moon and star’ appearance in watermelon

Author

Sen Yang, Junling Dou, Huayu Zhu, Dongming Liu, Jianbin Hu, Luming Yang, Jinfang Liang, Shouru Sun, and Dongling Sun

Subjects

0106 biological sciences, 0301 basic medicine, Chlorophyll content, Spots, food and beverages, Horticulture, Biology, Star (graph theory), 01 natural sciences, Genetic analysis, 03 medical and health sciences, 030104 developmental biology, Trait, Dominant inheritance, 010606 plant biology & botany

Abstract

Plant appearance is one of the most important characteristics affecting consumption and breeding choices. In watermelon, except for the normal phenotypes such as the basic foreground pattern (solid/stripe), background pattern (yellow/green rind), and fruit shape (round/oblong), there was a novel and unique appearance called ‘moon and star’ trait with big and tiny yellow spots on the fruit rind. Following a dominant inheritance pattern, the attracting appearance is convenient for variety breeding. The result of this study revealed that the chlorophyll content dramatically decreased and chloroplast structure significantly changed for the yellow spot, which were supposed to be the direct reason for fruit color change. Contrary to a previous study, genetic analysis showed that there were two interacting genes responsible for this novel trait. Using bulk segregant analysis, two candidate regions located on chromosome 1 and 8 were identified to contain these two genes regulating the ‘moon and star’ trait.

Published

2021