Your search keyword '"Kurbatov SA"' showing total 2 results

1. [Autosomal dominant spastic paraplegias].

Author

Rudenskaya GE, Kadnikova VA, Bessonova LA, Sparber PA, Kurbatov SA, Mironovich OL, Konovalov FA, and Ryzhkova OP

Subjects

Adolescent, Child, Heterozygote, Humans, Membrane Transport Proteins genetics, Mutation, Phenotype, GTP-Binding Protein gamma Subunits, Spastic Paraplegia, Hereditary diagnosis, Spastic Paraplegia, Hereditary genetics

Abstract

Objective: To estimate the proportion and spectrum of infrequent autosomal dominant spastic paraplegias in a group of families with DNA-confirmed diagnosis and to investigate their molecular and clinical characteristics., Material and Methods: Ten families with 6 AD-SPG: SPG6 ( n =1), SPG8 ( n =2), SPG9A ( n =1), SPG12 ( n =1), SPG17 ( n =3), SPG31 ( n =2) were studied using clinical, genealogical, molecular-genetic (massive parallel sequencing, spastic paraplegia panel, whole-exome sequencing, multiplex ligation-dependent amplification, Sanger sequencing) and bioinformatic methods., Results and Conclusion: Nine heterozygous mutations were detected in 6 genes, including the common de novo mutation p.Gly106Arg in NIPA1 (SPG6), the earlier reported mutation p.Val626Phe in WASHC5 (SPG8) in isolated case and the novel p.Val695Ala in WASHC5 (SPG8) in a family with 4 patients, the novel mutation p.Thr301Arg in RTN2 (SPG12) in a family with 2 patients, the novel mutation c.105+4A>G in REEP1 (SPG31) in a family with 4 patients and the reported earlier p.Lys101Lys in REEP1 (SPG31) in a family with 3 patients, the known de novo mutation p.Arg252Gln in ALDH18A1 (SPG9A) in two monozygous twins; the common mutation p.Ser90Leu in BSCL2 (SPG17) in a family with 3 patients and in isolated case, reported mutation p.Leu363Pro in a family with 2 patients. SPG6, SPG8, SPG12 and SPG31 presented 'pure' phenotypes, SPG31 had most benign course. Age of onset varied in SPG31 family and was atypically early in SPG6 case. Patients with SPG9A and SPG17 had 'complicated' paraplegias; amyotrophy of hands typical for SPG17 was absent in a child and in an adolescent from 2 families, but may develop later.

Published

2021

2. [Alarming signs and symptoms in the early diagnostics of late onset Pompe disease: super omnia clinica].

Author

Nikitin SS, Kurbatov SA, Bredelev VA, and Kovalchuk MO

Subjects

Adult, Aged, Diagnosis, Differential, Early Diagnosis, Female, Fluorometry, Glycogen Storage Disease Type II complications, Humans, Infant, Late Onset Disorders complications, Male, Middle Aged, Muscle Weakness diagnosis, Muscle Weakness etiology, Muscle, Skeletal physiopathology, alpha-Glucosidases deficiency, Glycogen Storage Disease Type II diagnosis, Glycogen Storage Disease Type II enzymology, Late Onset Disorders diagnosis, Late Onset Disorders enzymology, alpha-Glucosidases blood

Abstract

Pompe disease (PD) is a rare autosomal recessive muscle lysosomal glycogenosis caused by a deficiency of acid-α-glucosidase. There are two main forms of the disease: aggressive infantile PD started within the first year of life with a severe enzyme deficiency and multiorgan involvement, and late onset PD (LOPD) with progressive signs and symptoms including predominant proximal, axial muscle weakness and respiratory insufficiency started at any time from 1 till 75 years and older. Usually due to physician's unawareness, most adults with PD are diagnosed with great delay. The typical features and early nonspecific signs in four patients, aged between 35 and 72 years, with confirmed LOPD are delineated and discussed in correspondence with the age of first signs, age development of muscle weakness, distribution and age of final diagnosis. The disorders for differential diagnosis and spectrum of conditions that expanded the possibility of PB are listed. The fluorometrically analyzed level of acid α-glucosidase from dried blood spots is considered to be the first choice diagnostic method for clinically suspected cases of LOPD.

Published

2015