Your search keyword '"Breningstall G"' showing total 7 results

1. Skeletal Muscle Pathogenesis in Polyglutamine Diseases.

Author

Marchioretti, Caterina, Zuccaro, Emanuela, Pandey, Udai Bhan, Rosati, Jessica, Basso, Manuela, and Pennuto, Maria

Subjects

SKELETAL muscle, POLYGLUTAMINE, MUSCULAR atrophy, CENTRAL nervous system, SPINAL muscular atrophy, HUNTINGTON disease

Abstract

Polyglutamine diseases are characterized by selective dysfunction and degeneration of specific types of neurons in the central nervous system. In addition, nonneuronal cells can also be affected as a consequence of primary degeneration or due to neuronal dysfunction. Skeletal muscle is a primary site of toxicity of polyglutamine-expanded androgen receptor, but it is also affected in other polyglutamine diseases, more likely due to neuronal dysfunction and death. Nonetheless, pathological processes occurring in skeletal muscle atrophy impact the entire body metabolism, thus actively contributing to the inexorable progression towards the late and final stages of disease. Skeletal muscle atrophy is well recapitulated in animal models of polyglutamine disease. In this review, we discuss the impact and relevance of skeletal muscle in patients affected by polyglutamine diseases and we review evidence obtained in animal models and patient-derived cells modeling skeletal muscle. [ABSTRACT FROM AUTHOR]

Published

2022

2. DFNA20/26 and Other ACTG1-Associated Phenotypes: A Case Report and Review of the Literature.

Author

Sorrentino, Ugo, Piccolo, Chiara, Rigon, Chiara, Brasson, Valeria, Trevisson, Eva, Boaretto, Francesca, Martini, Alessandro, and Cassina, Matteo

Subjects

PHENOTYPES, LITERATURE reviews, CONGENITAL disorders, HEARING disorders, HAIR cells, AUDITORY neuropathy

Abstract

Since the early 2000s, an ever-increasing subset of missense pathogenic variants in the ACTG1 gene has been associated with an autosomal-dominant, progressive, typically post-lingual non-syndromic hearing loss (NSHL) condition designed as DFNA20/26. ACTG1 gene encodes gamma actin, the predominant actin protein in the cytoskeleton of auditory hair cells; its normal expression and function are essential for the stereocilia maintenance. Different gain-of-function pathogenic variants of ACTG1 have been associated with two major phenotypes: DFNA20/26 and Baraitser-Winter syndrome, a multiple congenital anomaly disorder. Here, we report a novel ACTG1 variant [c.625G>A (p. Val209Met)] in an adult patient with moderate-severe NSHL characterized by a downsloping audiogram. The patient, who had a clinical history of slowly progressive NSHL and tinnitus, was referred to our laboratory for the analysis of a large panel of NSHL-associated genes by next generation sequencing. An extensive review of previously reported ACTG1 variants and their associated phenotypes was also performed. [ABSTRACT FROM AUTHOR]

Published

2021

3. De Novo ACTG1 Variant Expands the Phenotype and Genotype of Partial Deafness and Baraitser–Winter Syndrome.

Author

Dawidziuk, Mateusz, Kutkowska-Kazmierczak, Anna, Bukowska-Olech, Ewelina, Jurek, Marta, Kalka, Ewa, Guilbride, Dorothy Lys, Furmanek, Mariusz Ireneusz, Bekiesinska-Figatowska, Monika, Bal, Jerzy, and Gawlinski, Pawel

Subjects

GENOTYPES, SENSORINEURAL hearing loss, EXOMES, MOLECULAR diagnosis, GENETIC disorders, DUAL diagnosis, PHENOTYPES

Abstract

Actin molecules are fundamental for embryonic structural and functional differentiation; γ-actin is specifically required for the maintenance and function of cytoskeletal structures in the ear, resulting in hearing. Baraitser–Winter Syndrome (B-WS, OMIM #243310, #614583) is a rare, multiple-anomaly genetic disorder caused by mutations in either cytoplasmically expressed actin gene, ACTB (β-actin) or ACTG1 (γ-actin). The resulting actinopathies cause characteristic cerebrofrontofacial and developmental traits, including progressive sensorineural deafness. Both ACTG1-related non-syndromic A20/A26 deafness and B-WS diagnoses are characterized by hypervariable penetrance in phenotype. Here, we identify a 28th patient worldwide carrying a mutated γ-actin ACTG1 allele, with mildly manifested cerebrofrontofacial B-WS traits, hypervariable penetrance of developmental traits and sensorineural hearing loss. This patient also displays brachycephaly and a complete absence of speech faculty, previously unreported for ACTG1-related B-WS or DFNA20/26 deafness, representing phenotypic expansion. The patient's exome sequence analyses (ES) confirms a de novo ACTG1 variant previously unlinked to the pathology. Additional microarray analysis uncover no further mutational basis for dual molecular diagnosis in our patient. We conclude that γ-actin c.542C > T, p.Ala181Val is a dominant pathogenic variant, associated with mildly manifested facial and cerebral traits typical of B-WS, hypervariable penetrance of developmental traits and sensorineural deafness. We further posit and present argument and evidence suggesting ACTG1-related non-syndromic DFNA20/A26 deafness is a manifestation of undiagnosed ACTG1-related B-WS. [ABSTRACT FROM AUTHOR]

Published

2022

4. Acute Movement Disorders in Childhood.

Author

Garone, Giacomo, Graziola, Federica, Grasso, Melissa, and Capuano, Alessandro

Subjects

MOVEMENT disorders, NEUROLOGICAL emergencies, PEDIATRIC neurology, MEDICAL personnel, GENETIC disorders

Abstract

Acute-onset movement disorders (MDs) are an increasingly recognized neurological emergency in both adults and children. The spectrum of possible causes is wide, and diagnostic work-up is challenging. In their acute presentation, MDs may represent the prominent symptom or an important diagnostic clue in a broader constellation of neurological and extraneurological signs. The diagnostic approach relies on the definition of the overall clinical syndrome and on the recognition of the prominent MD phenomenology. The recognition of the underlying disorder is crucial since many causes are treatable. In this review, we summarize common and uncommon causes of acute-onset movement disorders, focusing on clinical presentation and appropriate diagnostic investigations. Both acquired (immune-mediated, infectious, vascular, toxic, metabolic) and genetic disorders causing acute MDs are reviewed, in order to provide a useful clinician's guide to this expanding field of pediatric neurology. [ABSTRACT FROM AUTHOR]

Published

2021

5. CHD2-Related CNS Pathologies.

Author

Wilson, Marc-Michel, Henshall, David C., Byrne, Susan M., and Brennan, Gary P.

Subjects

DNA-binding proteins, GENETIC mutation, DNA helicases, PATHOLOGY, DEVELOPMENTAL delay, INTELLECTUAL disabilities, DNA replication

Abstract

Epileptic encephalopathies (EE) are severe epilepsy syndromes characterized by multiple seizure types, developmental delay and even regression. This class of disorders are increasingly being identified as resulting from de novo genetic mutations including many identified mutations in the family of chromodomain helicase DNA binding (CHD) proteins. In particular, several de novo pathogenic mutations have been identified in the gene encoding chromodomain helicase DNA binding protein 2 (CHD2), a member of the sucrose nonfermenting (SNF-2) protein family of epigenetic regulators. These mutations in the CHD2 gene are causative of early onset epileptic encephalopathy, abnormal brain function, and intellectual disability. Our understanding of the mechanisms by which modification or loss of CHD2 cause this condition remains poorly understood. Here, we review what is known and still to be elucidated as regards the structure and function of CHD2 and how its dysregulation leads to a highly variable range of phenotypic presentations. [ABSTRACT FROM AUTHOR]

Published

2021

6. The Differences in the Diagnostic Profile in Children with Vasovagal Syncope between the Result of Head-Up Tilt Table Test.

Author

Kolarczyk, Ewelina, Szydłowski, Lesław, Skierska, Agnieszka, and Markiewicz-Łoskot, Grażyna

Published

2020

7. Actin Mutations and Their Role in Disease.

Author

Parker, Francine, Baboolal, Thomas G., and Peckham, Michelle

Subjects

EUKARYOTIC cells

Abstract

Actin is a widely expressed protein found in almost all eukaryotic cells. In humans, there are six different genes, which encode specific actin isoforms. Disease-causing mutations have been described for each of these, most of which are missense. Analysis of the position of the resulting mutated residues in the protein reveals mutational hotspots. Many of these occur in regions important for actin polymerization. We briefly discuss the challenges in characterizing the effects of these actin mutations, with a focus on cardiac actin mutations. [ABSTRACT FROM AUTHOR]

Published

2020