PHI with Neuromyelitis optica

Acute attacks typically last from several days to several weeks, with symptoms developing rapidly.

A chronic, relapsing-remitting disease. Without long-term preventative treatment, attacks can occur frequently over a lifetime, leading to cumulative disability.

High, ranging from several thousands to tens of thousands of dollars for acute attack management (e.g., high-dose corticosteroids, plasma exchange, IVIg), often requiring hospitalization.

Very high, potentially hundreds of thousands to millions of dollars over a lifetime due to chronic immunosuppressive therapy, frequent monitoring, managing residual disabilities, rehabilitation, and potential hospitalizations for relapses.

Historically significant (up to 30% within 5-10 years without treatment, often due to respiratory failure from severe spinal cord or brainstem lesions). With modern treatment, mortality is substantially reduced but remains higher than the general population.

Very high. Each attack often causes permanent damage, leading to residual deficits such as severe vision loss or blindness, paralysis, chronic pain, spasticity, bladder/bowel dysfunction, and cognitive impairment. Significant psychological impact is also common.

Low, especially after severe attacks. Partial recovery is common, but complete recovery without any residual neurological deficits is rare, and recovery tends to be less complete than in diseases like Multiple Sclerosis.

While NMOSD itself is often defined by specific autoantibodies (AQP4-IgG or MOG-IgG), there is an increased probability of co-occurrence with other autoimmune diseases, such as Systemic Lupus Erythematosus (SLE) or Sjögren's Syndrome, in a subset of patients.