Abstract
Dilated cardiomyopathy (DCM) is a complex, etiologically heterogeneous myocardial disease, which is one of the main causes of heart failure and heart transplantation. In 2016, experts from the European working group proposed a new definition of cardiomyopathy, which includes intermediate variants with a change in phenotype in carriers of mutations from subclinical form to the full manifestations of the disease. The classification of DCM was supplemented with intermediate phenotypes with the inclusion of a hypokinetic form with reduced contractile function without ventricular dilatation and variants with predominant dilation or arrhythmogenicity. Pathological architectonics of DCM consists of many genetic determinants that interact with numerous environmental factors. Clinical manifestations depend not only on the malignancy and penetrance of the gene mutation, but also on a number of other causes — epigenomic factors, age, toxic effects, environmental aggressiveness, pregnancy, and the effects of other acquired diseases. The article summarizes the current epidemiological data and ideas about specific molecular changes with an unfavorable prognosis. For clarity, we present clinical observations of familial DCM with mutations in the RBM20 and LMNA genes.
Highlights
In 2016, experts from the European working group proposed a new definition of cardiomyopathy, which includes intermediate variants with a change in phenotype in carriers of mutations from subclinical form to the full manifestations of the disease
The classification of Dilated cardiomyopathy (DCM) was supplemented with intermediate phenotypes with the inclusion of a hypokinetic form with reduced contractile function without ventricular dilatation and variants with predominant dilation or arrhythmogenicity
Pathological architectonics of DCM consists of many genetic determinants that interact with numerous environmental factors
Summary
У многих родственников пробандов, которые являются носителями патогенных мутаций, существует доклиническая стадия (иногда длительная) без выраженных структурно-функциональных проявлений болезни, которая впоследствии прогрессирует к изолированной дилатации ЛЖ (присутствует у 25% родственников с семейной формой ДКМП, и позже развивается полный фенотип в последующие годы) или к аритмогенному фенотипу (желудочковые или наджелудочковые аритмии, дефекты проводимости), который может наблюдаться на ранней стадии генетических заболеваний, например, при мутациях в гене ламина A/C, десмина или при нейромышечной патологии [9,10,11]. Стадия систолической дисфункции обычно связана с дилатацией ЛЖ, но в некоторых ситуациях (как у носителей мутаций в генах ламина A/C, десмина, а также у некоторых пациентов с неизвестной генетической причиной [9,10,11,12,13]) дилатация ЛЖ может отсутствовать; поэтому во избежание диагностической путаницы эксперты предложили новый промежуточный фенотип ДКМП — гипокинетическую кардиомиопатию без дилатации желудочков (HNDC или DCM [ND-H]). Генотип-фенотипические корреляции при ДКМП еще точно не определены, Химиотерапия (антрациклины, моноклональная терапия)
Sign-in/Register to view highlights & summary Sign-in/Register to access full text options 
Talk to us
Join us for a 30 min session where you can share your feedback and ask us any queries you have
Schedule a callDisclaimer: All third-party content on this website/platform is and will remain the property of their respective owners and is provided on "as is" basis without any warranties, express or implied. Use of third-party content does not indicate any affiliation, sponsorship with or endorsement by them. Any references to third-party content is to identify the corresponding services and shall be considered fair use under The CopyrightLaw.
