Your search keyword '"Sparber, Peter"' showing total 3 results

1. Specificities of the DMD Gene Mutation Spectrum in Russian Patients.

Author

Zinina, Elena, Bulakh, Maria, Chukhrova, Alena, Ryzhkova, Oksana, Sparber, Peter, Shchagina, Olga, Polyakov, Aleksander, and Kutsev, Sergey

Subjects

BECKER muscular dystrophy, GENETIC mutation, LIMB-girdle muscular dystrophy, MUSCULAR dystrophy, CREATINE kinase, FACIOSCAPULOHUMERAL muscular dystrophy

Abstract

Duchenne/Becker muscular dystrophy (DMD/BMD) is the most common form of muscular dystrophy, accounting for over 50% of all cases. In this regard, in Russia we carry out a program of selective screening for DMD/BMD, which mainly involves male patients. The main inclusion criteria are an increase in the level of creatine phosphokinase (>2000 U/L) or an established clinical diagnosis. At the first stage of screening, patients are scanned for extended deletions and duplications in the DMD gene using multiplex ligase-dependent probe amplification (MLPA SALSA P034 and P035 DMD probemix, MRC-Holland). The second stage is the search for small mutations using a custom NGS panel, which includes 31 genes responsible for various forms of limb-girdle muscular dystrophy. In a screening of 1025 families with a referral Duchenne/Becker diagnosis, pathogenic and likely pathogenic variants in the DMD gene were found in 788 families (in 76.9% of cases). In the current study, we analyzed the mutation spectrum of the DMD gene in Russian patients and noted certain differences between the examined cohort and the multi-ethnic cohort. The analysis of the DMD gene mutation spectrum is essential for patients with DMD/BMD because the exact mutation type determines the application of a specific therapeutic method. [ABSTRACT FROM AUTHOR]

Published

2022

2. Retrospective analysis of 17 patients with mitochondrial membrane protein-associated neurodegeneration diagnosed in Russia.

Author

Sparber, Peter, Krylova, Tatiana, Repina, Svetlana, Demina, Nina, Rudenskaya, Galina, Sharkova, Inna, Sharkov, Artem, Kadyshev, Vitaly, Kanivets, Ilya, Korostelev, Sergey, Pomerantseva, Ekaterina, Kaimonov, Vladimir, Mikhailova, Svetlana, Zakharova, Ekaterina, and Skoblov, Mikhail

Subjects

*MITOCHONDRIAL membranes, *RNA analysis, *NEURODEGENERATION, *DNA analysis, *CREATINE kinase, *SPASTICITY, *FAMILIAL spastic paraplegia, *BRAIN diseases, *BASAL ganglia, *RETROSPECTIVE studies, *MAGNETIC resonance imaging, *IRON metabolism disorders, *MEMBRANE proteins, *BRAIN stem

Abstract

Introduction: Mitochondrial membrane protein-associated neurodegeneration (MPAN) is a rare neurological syndrome caused by pathogenic variants in the C19orf12 and is characterized by iron deposition in the basal ganglia and substantia nigra. Only a limited number of cohort studies were published to date and the prevalence of MPAN remains uncertain.Methods: Recruited subjects with MPAN in Russia were diagnosed by whole-exome sequencing or Sanger sequencing of the C19orf12 gene. Data of over 14000 whole exome sequencing analyses was used to calculate the estimated disease frequency. RNA analysis was performed by RT-PCR. QSVanalyzer software was used to quantify the allelic disbalance.Results: We describe the clinical and molecular characterizations of 17 patients with MPAN. DNA analysis detected three previously undescribed pathogenic/likely pathogenic variants in the C19orf12 gene. The estimated disease frequency was calculated to be 1:619150. We describe unusual clinical observations in several cases. One patient showed severe neurogenic muscle weakness along with a lack of marked spasticity or optic nerve atrophy. In another mild clinical case with the NM_001031726.3:c.204_214del (p.(Gly69Argfs*10)) variant in a heterozygous state, a marked allelic disbalance was observed on the RNA level with reduced expression level of the wild-type allele. Thus, this case became the first one of a possible regulatory variant causing MPAN.Conclusion: We reported a detailed clinical and molecular characterization of the third-largest MPAN cohort. We expanded the mutational and clinical spectrum of MPAN. Moreover, we calculated the estimated MPAN frequency in the Russian population for the first time. [ABSTRACT FROM AUTHOR]

Published

2021

3. Recessive myotonia congenita caused by a homozygous splice site variant in CLCN1 gene: a case report.

Author

Sparber, Peter, Sharova, Margarita, Filatova, Alexandra, Shchagina, Olga, Ivanova, Evgeniya, Dadali, Elena, and Skoblov, Mikhail

Subjects

*NEUROMUSCULAR diseases, *CALF muscles, *MUSCLE growth, *CREATINE kinase, *FUNCTIONAL analysis, *PATHOLOGY

Abstract

Background: Myotonia congenita is a rare neuromuscular disease, which is characterized by a delay in muscle relaxation after evoked or voluntary contraction. Myotonia congenita can be inherited in a dominant (Thomsen disease) and recessive form (Becker disease) and both are caused by pathogenic variants in the CLCN1 gene. Noncanonical splice site variants are often classified as variants of uncertain significance, due to insufficient accuracy of splice-predicting tools. Functional analysis using minigene plasmids is widely used in such cases. Moreover, functional analysis is very useful in investigation of the disease pathogenesis, which is necessary for development of future therapeutic approaches. To our knowledge only one noncanonical splice site variant in the CLCN1 gene was functionally characterized to date. We further contribute to this field by evaluation the molecular mechanism of splicing alteration caused by the c.1582 + 5G > A in a homozygous state. Case presentation: We report a clinical case of an affected 6-y.o boy with athletic appearance due to muscle hypertrophy, calf muscle stiffness, cramping and various myotonic signs in a consanguineous family with no history of neuromuscular disorders. The neurological examination showed percussion-activated myotonia in the hands and legs. Plasma creatine kinase enzyme and transaminases levels were normal. Electromyography at the time of examination shows myotonic runs in the upper and lower extremities. Conclusions: Functional analysis of the variant in a minigene system showed alteration of splicing leading to loss of function, thereby confirming that the variant is pathogenic. [ABSTRACT FROM AUTHOR]

Published

2020