Symptoms typically begin in adulthood, often between the ages of 30 and 60, though some forms may present earlier or later. Common manifestations include muscle cramps, stiffness, weakness in the shoulders, hips, and pelvic region, and difficulty with activities such as climbing stairs or rising from a seated position. In advanced stages, respiratory or cardiac muscle involvement may occur, posing serious health risks. Some individuals also experience mild cognitive or sensory impairments, though these are less common.
Diagnosis relies on a combination of clinical evaluation, genetic testing, and muscle biopsy. Genetic testing can identify mutations in genes such as *MYOT*, *BAG3*, *DES*, or *FLNC*, which are frequently associated with myofibrillar myopathies. Muscle biopsy may reveal characteristic protein aggregates or structural abnormalities under microscopic examination. Electromyography (EMG) can help assess nerve and muscle function, though it is not definitive on its own.
There is currently no cure for mykvevdefekter, and treatment focuses on managing symptoms. Physical therapy and exercise, tailored to the individual’s capabilities, can help maintain muscle strength and mobility. Assistive devices, such as braces or walkers, may improve independence. In severe cases, respiratory support or cardiac monitoring may be required. Research into gene therapy and other experimental treatments is ongoing, offering potential future advancements for affected individuals.
The condition is typically inherited in an autosomal dominant or recessive pattern, meaning it can be passed from parent to child or arise from new mutations. Genetic counseling is recommended for families with a history of myofibrillar myopathies to assess risks and inform reproductive decisions. Support groups and multidisciplinary care teams play a crucial role in improving quality of life for those living with these disorders.