Abstract:
Introduction. In children, Progressive Muscular Dystrophies (PMD) are a wide group of genetic diseases which
affect skeletal muscles by progressive weakness and degeneration, caused by genetic alterations. In some cases,
involvement is not limited to muscles, but it may influence other organs, such as heart and respiratory muscles. This
category of pathologies causes progressive weakness and loss of muscle mass. In muscular dystrophy, abnormal
genes (mutations) interfere with the production of proteins needed to form healthy muscles. Histologically,
Progressive Muscular Dystrophies are unified by the presence of necrotic and regenerating processes, related with
an increased amount of connective and adipose tissues.
Aim of study. Elucidation and comprehensive overview of the clinical and genetic aspects of progressive muscular
dystrophies in children.
Methods and materials. The presented work was created on the basis of review of literature exploring bibliographic
sources, using manuals and articles published in databases: PubMed, Google Scholar, Medscape, NCBI,
ScienceDirect.
Results. The analysis and synthesis of literature and bibliographic sources show the existence of many types of
progressive muscular dystrophies. There are at least 16 different types of PMD in children. All of them are genetically
determined diseases of the muscles which lead to progressive weakness. According to the mode of transmission,
Progressive Muscular Dystrophies are classified in the following types (David Gardner-Medwin MD FRCP
classification): X-linked recessive muscular dystrophies: - Duchenne muscular dystrophy (severe type); - Becker
muscular dystrophy (benigne type); - Benign muscular dystrophy with early contractures; - Scapulo-peroneal
muscular dystrophy (Emery-Dreifuss); X-linked dominant muscular dystrophies: - Hereditary myopathy in females;
Autosomal recessive muscular dystrophies: - Scapulohumeral (limb-girdle) muscular dystrophy: LGMD2A-2W -
Quadriceps myopathy; - Childhood hereditary autosomal recessive myopathy; - Congenital muscular dystrophy; -
Adult distal muscular dystrophy: Nonaka, Miyoshi - Oculopharyngeal muscular dystrophy; Autosomal dominant
muscular dystrophies: - Scapulo-peroneal autosomal dominant muscular dystrophy; - Late-onset proximal autosomal
dominant muscular dystrophy; – Facioscapulohumeral muscular dystrophy (Landouzy-Dejerine). All these types are
distinguished based on some specific genetic mutations unique for each type of PMD characterised by a different
pattern of muscle distribution, different involvement of skeletal muscles, body organs and variable course of
evolution. The most important and frequent PMD are Duchenne progressive muscular dystrophy (DMD) and Becker
progressive muscular dystrophy (BMD). These are some of the most severe forms of progressive muscular
dystrophies in children. Nowadays, there is no effective treatment for DMD/BMD and other PMD. Despite
significant progress of molecular biology and genetics that has been achieved over the last two decades in this
domain, prevention, carrier detection, counselling, and prenatal diagnosis remain the only effective strategies against
these pathologies.
Conclusion. Progressive Muscular dystrophies (PMD) represent a collective group of inherited non-inflammatory
but progressive muscle disorders with many phenotypic characteristics, which are difficult to diagnose in the early
stage of the disease. Elucidation of clinical and genetic aspects are essential for prevention, establishment of an
accurate diagnosis, genetic counselling of families in the high-risk group and prenatal diagnosis for prophylaxis. It
is important to know the clinical and laboratory aspects in PMD to detect these diseases as early as possible and to
apply therapeutic protocols in order to increase life expectancy, thus improving the quality of these patients' lives
and of their families.