Abstract
Human metapneumovirus (hMPV) is a nonsegmented, single-stranded, negative-sense RNA virus belonging to the Pneumoviridae family. It was first identified in 2001 in the nasopharyngeal secretions of 28 Dutch children with bronchiolitis collected over a 20-year period. hMPV exhibited paramyxovirus-like morphology with many genetic similarities to respiratory syncytial virus. hMPV has 1 serotype with 2 major subgroups (A and B) and 5 sublineages (A1, A2a, A2b, B1, and B2). In the wake of its discovery, a wealth of observational research has demonstrated global circulation of hMPV causing a wide spectrum of clinical disease. It accounts for 2% to 7% of all symptomatic respiratory infections in children who are universally infected by age 5 years. However, long-lasting immunity to hMPV is incomplete, and reinfections occur throughout life. With increasing age, the impact of hMPV is greater. Adult patients with hMPV infection may develop pneumonia, resulting in hospitalization and severe outcomes, such as intensive care unit admission or mechanical ventilation. Risk factors for severe hMPV are still being defined but include profound immunosuppression (20%), congestive heart failure (25%), and severe chronic obstructive pulmonary disease (20%). In this supplement, several studies from diverse geographic and clinical locations explore the pathogenesis, epidemiology, and clinical profile of hMPV as compared with respiratory syncytial virus and/or influenza and examine the impact of risk factors for severe disease, including age and chronic comorbid conditions. These data are needed to provide the basis for understanding who might benefit from future hMPV vaccines.