Endocardial fibroelastosis is characterized by diffuse endocardial thickening and myocardial dysfunction. The endocardial thickening is believed to be caused by persistent and increased wall tension in the ventricles, possibly secondary to damaged myocardium, mitral regurgitation, or both. It presents as unexplained heart failure in infants and children.
The disease can be primary or secondary to various congenital heart diseases, most notably hypoplastic left heart syndrome, aortic stenosis, or atresia. The two pathologic forms of primary endocardial fibroelastosis include dilated, which is most common, and contracted.
Primary endocardial fibroelastosis is not associated with any significant structural anomaly of the heart. Secondary endocardial fibroelastosis is associated with other congenital heart diseases. Once regarded as a common cause of unexplained heart failure, endocardial fibroelastosis is now considered rare.
Endocardial fibroelastosis presents during the first 3-6 months of life in 80% of cases. The typical age at diagnosis is 2-12 months. Endocardial fibroelastosis is rarely reported in adolescents and adults and is an important cause of nonimmune hydrops fetalis.
The disease is usually sporadic, but familial cases have been reported (10%). Observations that favor a viral etiology include a clinical presentation similar to that of chronic myocarditis, findings of myocarditis or myocardial fibrosis in affected patients, a higher incidence following epidemics of coxsackievirus B infection, demonstration of persistent viral infection with molecular studies, and experimental production of the disease in animal models by viral infections of the myocardium. A phenotypic resemblance to dilated cardiomyopathy has been noted.
In approximately 50% of patients, the mitral and aortic valves are involved, often producing marked deformity and either valvar regurgitation or stenosis.
The less common contracted type of primary endocardial fibroelastosis is associated with a relatively hypoplastic or normal LV size. The right and left atria and the right ventricle are markedly enlarged and hypertrophied, with minimal or no endocardial sclerosis. An early event in fetal life is believed to result in dilated endocardial fibroelastosis, which later morphoses into a contracted type. This suggests that the dilated type could appear as 2 different diseases while remaining a single disease. Secondary endocardial fibroelastosis, associated with cardiac malformations, is attributed to the cardiac hypertrophy and consequent imbalance in the myocardial oxygen supply-demand relationship. Resultant fibroelastotic thickening is often focal and less severe.
Acute congestive heart failure (CHF) becomes progressive CHF that results in death within weeks, usually within the first 6 months of life. In a subgroup of individuals who survive from a few months to several years, a more chronic course is common. Such patients respond to medications used to treat CHF. A variable cyclical clinical course ensues, with CHF recurrences related to respiratory or other intercurrent infections or to progression of disease. Remissions can occur with intensification of medical therapy.
A 1964 study demonstrated an incidence rate of 1 per 5,000 live births in the United States. The incidence over subsequent years has been markedly reduced for unknown reasons, with almost no new cases in the current era. The disappearance of this condition is believed to be related to the declining prevalence of mumps.
An International 1978 study reported that endocardial fibroelastosis comprised 1-2% of all congenital heart diseases. Currently, the number of endocardial fibroelastosis cases has dramatically fallen to almost zero. The idiopathic form of the disease is sporadic, but familial cases are also reported (10%).
Progressive CHF causes deteriorating conditions that lead to death in one third of patients. One third of the patients survive and may experience persistent symptoms or have residual ECG abnormalities or evidence of cardiomegaly. Although some authorities are skeptical, some believe that approximately one third of the patients completely recover. Early diagnosis and prompt persistent administration of digitalis may result in clinical improvement and reversion of the cardiac enlargement (CE) to normal.
Morbidity varies depending on presentation. Infants who present with acute failure almost always die from the acute episode unless they receive a transplant. Patients with a chronic presentation have a 30-40% mortality rate due to resistant heart failure. Contracted endocardial fibroelastosis has a grave prognosis and is generally fatal.