key: cord-0745817-p4hm5ih1 authors: Ramsey, Clare D.; Kumar, Anand title: Influenza and Endemic Viral Pneumonia date: 2013-10-02 journal: Crit Care Clin DOI: 10.1016/j.ccc.2013.06.003 sha: 8a13215dea9eeb9b5b7e7dfcc9f6ccfcbd3cb7e5 doc_id: 745817 cord_uid: p4hm5ih1 Viruses are a common and important cause of severe community-acquired pneumonia, and may lead to severe respiratory disease and admission to the intensive care unit. Influenza is the most common virus associated with severe viral pneumonia, although other important causes include respiratory syncytial virus, adenovirus, metapneumonia virus, and coronaviruses. Viral pneumonias tend to have a seasonal predilection and are often preceded by a typical viral prodrome. This article focuses on severe influenza pneumonia, including the 2009 H1N1 pandemic, and briefly discusses other causes of severe respiratory disease of viral etiology. saturations on high-level oxygen, radiographic characteristics, and lack of CHF would fit the description of acute respiratory distress syndrome (ARDS) secondary to viral pneumonia, as seen with the 2009 H1N1 pandemic. Many believe that much of the excess mortality attributed to the 1918 influenza epidemic was related to secondary bacterial pneumonia with organisms such as Staphylococcus aureus and Streptococcus pneumoniae. 5, 15 This opinion is supported by autopsy studies reporting severe bronchopneumonia with an ARDS-like illness, and cultured bacteria associated with pneumonic lesions; however, in some cases there was no evidence of bacterial pneumonia. 11, 16, 17 Good epidemiologic evidence supports the emergence of an antigenically novel influenza virus in 1918 with high virulence to which many younger people had never been exposed, which was likely a significant contributor to the high mortality rates in this younger age group. 12 In addition to the complication of severe respiratory failure, influenza infection has been associated with central nervous system, cardiac, skeletal, renal, and hepatic complications. 18 In the spring of 2009, an outbreak attributed to a new viral pathogen, swine-origin influenza A (2009 H1N1), led to a significant number of cases of severe hypoxemic respiratory failure attributable to viral pneumonia. The outbreak began in the Southwestern United States and Mexico, with rapid spread throughout the rest of the United States, Canada, and then the rest of the world. This spread led the World Health Organization (WHO) to declare a phase-6 global pandemic alert on June 11, 2009. 19 The number of patients requiring admission to an ICU for viral pneumonitis caused by 2009 H1N1 infection was much larger than rates due to seasonal influenza. 20 The increased incidence of critical illness, along with a high transmissibility rate and rapid increase in case numbers over a short period of time, created a significant stress on hospital resources in several countries, particularly in terms of ICU resources. 20, 21 The need for invasive ventilatory support in some relatively underresourced nations in the Western hemisphere reportedly exceeded ICU capacity (Farmer C, personal communication, 2010). Since the onset of the pandemic in March of 2009, more than 214 countries and communities reported cases of pandemic 2009 H1N1 influenza, with more than 18,000 deaths. 22 In Australian provinces, approximately 5% of the population developed H1N1-related illness, 0.3% of infected patients were hospitalized, and 20% of hospitalized patients required ICU care, very similar to the proportions reported by the Public Health Agency of Canada. 23, 24 During the pandemic in Argentina there were 1,390,566 cases of influenza-like illness and of those, 14,034 were admitted to hospital and 617 (4.4%) died as of January 2, 2010. 25 In the United Kingdom 13% of 2009 H1N1 patients, both adults and children, were admitted to either an ICU or highdependency unit, with a mortality rate of 5%. Of those who died, 59% were previously healthy, and hospital mortality rate increased with increasing age. 26 Overall the casefatality rate was low (<0.5%), and lower than generally reported for seasonal influenza, although there is much variability in estimates. [27] [28] [29] [30] [31] The viral epidemic was initially suspected after an increasing number of young patients in Mexico were hospitalized with severe and, not infrequently, fatal pneumonia. In a reported series of the initial 2155 cases of severe pneumonia in Mexico, Chowell and colleagues 32 found that 87% of deaths and 71% of cases of severe pneumonia occurred in patients between ages of 5 and 59 years, which represented a significant shift in the age distribution of patients with severe disease or deaths from seasonal influenza. In Australia and New Zealand, 722 patients were admitted to an ICU within a 3-month period of time with confirmed 2009 H1N1. The mean number of admissions for viral pneumonitis within the same period in the prior 4 years was 57. 33 Despite the young age of patients requiring ICU admission for respiratory failure, the highest death rate was among those older than 50 years. [34] [35] [36] However, because in comparison with seasonal influenza, 2009 H1N1 affected younger individuals, the number of years of life lost was substantial, estimated to be between 334,000 and 1973,000 years in the United States from May to December 2009. 37 Among those requiring critical care in Canada, 67% were female with a mean age of 32 years. The majority of patients had at least 1 comorbidity, most commonly chronic lung disease (asthma, chronic obstructive pulmonary disease [COPD], bronchopulmonary dysplasia), obesity, hypertension, smoking, and diabetes. However, the majority did not have the kinds of major chronic organ failure typical of patients admitted to medical ICUs. The mean Acute Physiology and Chronic Health Evaluation II (APACHE II) score of ICU patients was 20, with major comorbidities present in 30%. 21 Similar patient demographics were noted in other countries, and many are known risk factors for influenza infection. 33, 38, 39 Indigenous persons from Australia and New Zealand, as well as Aboriginal Canadians (26%), were overrepresented among those who were critical ill. 21, 33, 40 Obesity, which interestingly has not been previously linked to complications of influenza, was a prominent risk factor for severe respiratory disease secondary to 2009 H1N1. 21, 26, 33, 35, 38, [40] [41] [42] Pregnancy is well described as a risk factor for complications from seasonal influenza; however, the number of critically ill pregnant women with 2009 H1N1 pneumonitis was disproportionately large and led to excess mortality in this group. [42] [43] [44] [45] In Australia and New Zealand, pregnant women had a relative risk of 13.2 of requiring ICU admission for their illness in comparison with nonpregnant women of childbearing age. Sixty-nine percent of women required mechanical ventilation and 11% died, all with viral pneumonitis and ARDS. 44 In California, 22% of pregnant women infected by 2009 H1N1 required ICU admission and 8% died, leading to an influenza-specific maternal mortality rate of 4.3 per 100,000 live births. 46 Finally, factors associated with treatment were shown to correlate with severe disease. Canadian data showed that the interval from onset of symptoms to initiation of antiviral therapy or hospitalization was longer among patients with more severe disease (ICU admission or death), 24, 40 and this was also shown to be true among hospitalized patients in the United States. 35, 41 Observational studies of severe influenza H1N1 pneumonia suggest that early initiation of antiviral therapy is associated with improved outcomes. 47 Although most cases of 2009 H1N1 were mild and self-limited, there were a significant number of cases with severe hypoxemic respiratory failure. Five clinical presentations with 2009 H1N1 were commonly noted: viral pneumonitis, exacerbations of asthma or COPD, exacerbations of other underlying disease (ie, CHF, chronic renal disease), secondary bacterial pneumonia, and croup/bronchiolitis in the pediatric population. The clinical presentation most frequently requiring ICU admission was that of viral pneumonitis, and most of these patients presented with rapidly progressive and refractory hypoxemia and bilateral alveolar infiltrates on CXR. Most of these patients fulfilled criteria for acute lung injury (ALI) or ARDS. 25, 48 Patients with viral pneumonitis and hypoxemic respiratory failure presented with symptoms of cough, dyspnea, and fever. These patients had rapidly progressive hypoxemia with high ventilatory demands, and in most case series greater than 70% to 80% of patients admitted to the ICU with this syndrome required mechanical ventilation. 21, 35, 41, [49] [50] [51] Patients who presented with severe respiratory illness were hospitalized within a median of 2 to 6 days from onset of symptoms, and most requiring ICU admission did so within 24 hours of hospital admission. 21, 25, 39, 41, 49 In comparison with other causes of viral pneumonitis or seasonal influenza, an increased number of patients had gastrointestinal symptoms, typically diarrhea. 35, 41, [52] [53] [54] [55] The most common radiologic findings were bilateral patchy consolidation and/or ground-glass opacities, often worse in the lower lung zones (Fig. 1) . 56 Among those requiring ICU admission and ventilation, at least 3 out of 4 lung quadrants on CXR were most commonly involved. 21, 25, 39, 56 Computed tomography scans of the chest showed similar findings, with predominantly diffuse ground-glass infiltrates and consolidation. 56 In Canada, ICU patients with 2009 H1N1 pneumonitis had a mean PaO 2 /fraction of inspired oxygen (FiO 2 ) on admission of 147 mm Hg, and this remained on average lower than 200 among those remaining in the ICU at day 14. Seventy-three percent of patients had ALI at the onset of critical illness. Additional oxygenation and ventilatory support measures were not infrequently used, including high-frequency oscillatory ventilation (12%), nitric oxide (14%), neuromuscular blockade (30%), prone ventilation (5%), and extracorporeal membrane oxygenation (7%). 21 A similar degree Influenza and Viral Pneumonia of severe hypoxemia was noted in multiple case series from other countries. 25, 38, 49, 57 Thoracic compliance was noted to be decreased in a subset of patients with 2009 H1N1-related hypoxemic respiratory failure, with a median of 22 mL/cm H 2 O (interquartile range 21-34 mL/cm H 2 O). 38 A significant number of patients developed at least 1 other organ dysfunction, and in some cases developed multisystem organ dysfunction. 21, 38, 39 Duration of ventilation for 2009 H1N1 varied, with an average (median or mean reported) of 7 to 18 days. 21, 38, 51, 52, 58 The most common causes of death were severe ARDS with refractory hypoxemia and complications related to this, including infection, sepsis, or multisystem organ dysfunction. The most common infectious complication was secondary bacterial pneumonia, most frequently attributed to S aureus or S pneumoniae. 21, 35, 59 Diagnosis of 2009 H1N1 2009 pneumonitis is made based on the compatible clinical syndrome as already described, and the detection of the H1N1 influenza virus by RT-PCR and/or viral culture. Viral cultures take up to 1 week for processing and thus RT-PCR, typically on nasopharyngeal swabs, is the preferred technique. During the 2009 H1N1 pandemic, it was noted that false-negative nasopharyngeal aspirates occurred in more than 10% of patients with viral pneumonitis. In severe cases of illness, tracheal aspirates or bronchoalveolar lavage specimens from intubated patients and repeated collection are recommended to increase the PCR diagnostic yield. 23, 29 Pathophysiology Whether ARDS secondary to 2009 H1N1 is related to direct damage from the virus or to the host's immune response to the virus is unclear. Pandemic 2009 H1N1 virus can replicate in both the upper and the lower respiratory tract in comparison with seasonal influenza, which predominantly replicates in the upper respiratory tract. [60] [61] [62] In a retrospective study from Hong Kong, To and colleagues 63 examined the pattern of clinical disease, viral load, and immunologic profile between patients with varying severity of 2009 H1N1. Those who died or had ARDS had delayed clearance of viral load in their nasopharynx, had higher levels of proinflammatory cytokines and chemokines, and higher likelihood of viremia. There was significant correlation between the levels of interleukin (IL-6, IL-10, and IL-15) and disease severity. The association between high IL-6 and severe disease from influenza has been previously established. 64 Initial nasopharyngeal or endotracheal viral loads were similar among patients with differing disease severity; therefore, it would not appear to be viral load at the onset of infection that determines disease severity. 63 Most patients died of multisystem organ failure following admission for severe ARDS. On macroscopic examination, the lungs were noted to be heavy and diffusely edematous with areas of consolidation and hemorrhage. 65 Lung pathology typically showed diffuse alveolar damage (DAD), at times with associated areas of hemorrhage and necrotizing bronchiolitis (Figs. 2 and 3) . In a report from the Centers for Disease Control and Prevention (CDC) the most frequent histopathology in the airways of patients with 2009 H1N1 was inflammation and edema, with less frequent necrosis of the epithelium and hemorrhage. Lung tissue in all cases showed various stages of DAD, including edema, hyaline membranes, inflammation, and fibrosis. Seventeen patients had pulmonary thromboemboli. Immunohistochemistry showed viral antigens in airway epithelial cells, submucosal glands, and pneumocytes. 66 Viral antigen was also commonly seen in alveolar macrophages. 67 These studies show that H1N1 2009 virus has the ability to target both lower and upper respiratory tract infections, thus leading to DAD and clinical ARDS. Overall the pathologic findings were fairly similar to those published in autopsy studies from prior influenza epidemics in 1918 and 1957, including evidence of superimposed bacterial pneumonia. 13, 14, 68, 69 Several studies examining risk factors for the development of ARDS related to 2009 H1N1 noted that time to treatment with antivirals was important: patients who received appropriate antiviral therapy with oseltamivir or zanamavir shortly after presentation for medical care had better outcomes. 41, 46, 48 Rapid initiation of antivirals when H1N1 infection is suspected is particularly important in those with risk factors for disease progression and those requiring hospitalization. Ideally, therapy should be started within 48 hours of symptom onset, but is also effective and recommended if given later than this. 70 The recommended dose is 75 mg twice a day, although higher doses were given at some centers for critically ill and obese patients according to WHO recommendations. 71 Recent data suggest that 75 mg of oseltamivir administered twice per day via the orogastric route in critically ill patients consistently yields sufficient blood levels for near maximal (in vitro) suppression of viral replication. 72 Most patients also received broad-spectrum antimicrobial therapy, at least initially, while investigations were pending to determine the cause of respiratory failure. Current recommendations from the CDC state that antiviral treatment is recommended as early as possible in any patient with confirmed or suspected influenza who requires hospitalization, has severe, complicated, and progressive illness, or is at high risk for influenza complications (ie, <2 years and >65 years, immunocompromised, chronic disease, pregnant or postpartum, morbidly obese, Aboriginal, and residents of nursing homes or long-term care facilities). The current recommended therapy is either oseltamivir or inhaled zanamivir. However, in individuals with underlying respiratory disease, oseltamivir is recommended over zanamivir. 73 In critically ill patients with pneumonia, the viral RNA may be detected in lower airway secretions for several weeks after the initiation of oseltamivir. In patients with influenza pneumonia or evidence of clinical progression, an increased dose of the oseltamivir (150 mg twice daily in adults) and, more importantly, an increased duration of therapy for 10 days instead of 5 days, may be warranted. 29, 74 Oseltamivir-resistant viruses have been isolated, but are not common. The resistance is via a His275Tyr mutation in viral neuraminidase, which confers high-level resistance to oseltamivir but not zanamivir. Most resistant isolates have been found in patients with prior oseltamivir exposure, and have been associated with mild self-limited disease. If oseltamivir resistance is suspected or confirmed, treatment should be with zanamivir. 29, 75 Most patients admitted to an ICU with 2009 H1N1 viral pneumonitis fulfilled the criteria for ALI or ARDS and required mechanical ventilation. Many patients initiated on noninvasive positive-pressure ventilation (NIPPV) failed this mode, and subsequently required intubation and invasive ventilation. 21, 38 There are some reports of successful use of NIPPV, likely related to selection of less hypoxemic patients for this mode of treatment. 25 Concerns arose regarding transmission of H1N1 with NIPPV, as this mode of ventilation generates respiratory droplets and aerosols, which can reach a 0.5-m radius surrounding a patient receiving NIPPV. 76 Most centers internationally ventilated 2009 H1N1 viral pneumonitis patients with low tidal ventilation (6 mL/kg of predicted body weight and plateau pressures <30 cm H 2 O) whenever possible, as this is what has been recommended for ARDS based on results of the ARDSNet trial. 46, 69, 70, [77] [78] [79] High levels of positive endexpiratory pressure (PEEP) were noted to be required to manage severe hypoxemia, with mean PEEP levels between 16 and 22 cm H 2 O reported in some studies. 25, 38, 39, 49 Other modes of ventilation were also used, including airway pressure release ventilation and high-frequency oscillation; however, there are insufficient data to conclusively state whether these modes had any impact on outcomes. 21, 49 Similarly, recruitment maneuvers, prone positioning, and inhaled nitric oxide were used as salvage therapies for refractory hypoxemia, again with insufficient evidence to determine their effectiveness. 21, 25, 49, 80 Several studies have reported on the use of extracorporeal membrane oxygenation (ECMO) during the 2009 H1N1 pandemic. The largest of these series is from Australia, where 68 patients with severe ARDS (median PaO 2 /FiO 2 of 58 and PEEP of 18 cm H 2 O) were initiated on ECMO. Seventy-one percent survived their ICU admission and 21% died. By comparison, only 4 patients had been treated with ECMO for ARDS in the previous year in the same Australian centers. 58 Reports from other countries on the use of ECMO for ARDS related to H1N1 2009 pneumonia are much smaller, with mortality rates of between 56% and 67%. 81, 82 Avoidance of volume overload (and judicious diuresis) may also be associated with reduced duration of ventilation and length of stay in the ICU for most patients with ARDS. 83 This strategy was used and recommended in patients with ARDS related to 2009 H1N1. 84 Steroids were used in a variable number of patients across studies and for varying indications (sepsis, COPD or asthma exacerbation, stress-dose replacement therapy, or ARDS). 21, 41, 52 One study in Argentina examined the effect of treatment with corticosteroids, and found steroids to be safe and associated with improvement in lung injury score. However, there were only 13 patients and there was no real comparator group, as all patients received some degree of steroid therapy. 85 A study from the European Society of Intensive Care medicine H1N1 registry found that early use of corticosteroids in patients admitted to the ICU with H1N1 was associated with increased risk of superinfections, predominantly hospitalacquired pneumonia, with no mortality benefit. 86 Similarly, other studies found no mortality benefit or even harm with early steroid use. 87, 88 At present there is insufficient evidence for routine use of steroids in 2009 H1N1 or other influenza-related ARDS. Some historical data and experience with recent influenza epidemics suggests the potential utility of convalescent serum in the management of severe influenza. 89, 90 Although research on the issue is clearly required, the use of convalescent serum or immunoglobulin may become a useful treatment modality should future pandemic influenza A viruses be resistant to current antiviral agents. Adenovirus is a common cause of mild upper respiratory illness in children; however, up to 20% of all children who are infected with adenovirus develop pneumonia. 91 Among adults, adenovirus accounts for 1% to 7% of respiratory infections, particularly among immunocompromised adults and those in closed or crowed settings. 91, 92 Endemic cases occur throughout the year. In addition, epidemics have been reported among military recruits, long-term care facilities, and hospitals, with rapid spread of Influenza and Viral Pneumonia the virus. Adenovirus has also been shown to cause potentially fatal pneumonia, predominantly in immunocompromised hosts (especially transplant recipients). 93 Symptomatology is similar to that of other viral pneumonias, with fever, cough preceded by upper respiratory symptoms, and bilateral interstitial infiltrates on CXR. In cases of severe adenoviral pneumonia, case-fatality rates are high and may be above 50%. Most cases of adenoviral pneumonia are due to serotypes 3, 7, 11, or 14. Transmission occurs via respiratory droplet secretions, tears, fecal-oral spread, or environmental surfaces. Infection-control measures are paramount in limiting disease spread. 93, 94 The incubation period ranges from 2 to 14 days. Infections of the respiratory tract can also be associated with gastrointestinal symptoms (gastroenteritis or diarrhea). Detection of the virus is through PCR, serologic testing, or viral culture. PCR has the highest sensitivity and specificity, whereas viral culture can be insensitive and take up to 21 days. 91, 95 The treatment of adenovirus infections is supportive for mild disease; there are no approved antiviral drugs. Although often used in severe cases, ribavirin (a guanosine analogue) has not been shown to be effective in small clinical studies. 96 For immunocompromised patients and those with severe disease, cidofovir, a cytosine nucleotide analogue that inhibits DNA polymerase, has the greatest activity against the virus and is the preferred agent. 97 Several nonrandomized studies in hematopoietic stem cell transplant recipients have shown a favorable response to this agent. 98 Combination therapy with cidofovir and pooled intravenous immunoglobulin (IVIG) has been used, but data on the efficacy of this therapy are lacking. 98 The severe acute respiratory syndrome (SARS) coronavirus was first discovered in 2002/2003 when an epidemic originating in Southern China spread rapidly (in a limited number of cases) to the rest of Asia and then Europe, Canada, and the United States. SARS is a highly contagious virus, with high rates of spread identified in health care workers. The case-fatality rate during the epidemic was 9.6% and was strongly associated with increasing age (case-fatality rate of 43.3% in those older than 60 years). 99 SARS was noted to have multiple modes of transmission, including droplet and airborne spread as well as direct contact with contaminated surfaces. 100, 101 In the nosocomial cases, contaminated surfaces included surfaces in the patient's own rooms. The clinical presentation of SARS is one of a prolonged influenza-like prodrome of fever, cough, chills, myalgias, dyspnea, and headache. As the infection progresses the respiratory symptoms are more profound, and up to 20% of patients required ICU admission and mechanical ventilation after a median of 8 days from symptom onset. 102 The most common radiographic presentation was focal unilateral peripheral airspace disease, which progressed to multifocal unilateral or bilateral disease. 103, 104 Diagnosis is made based on clinical suspicion and contact with a known case, and is confirmed by either serologic testing or RT-PCR. RT-PCR for SARS has limited sensitivity and specificity, therefore repeated sampling is recommended. 105 As with influenza, tracheal aspirates may be helpful in intubated patients with severe pneumonia. Serologic testing is the most sensitive test but it takes several weeks for antibodies to develop, with a mean time to seroconversion of approximately 18 to 20 days. 106, 107 Treatment of SARS is supportive, with little evidence of any effective antivirals or other pharmacologic therapies. 108 A novel coronavirus was discovered in September 2012, which has now been referred to as the Middle East respiratory syndrome (MERS) coronavirus. As of May 31, 2013, 50 cases have been confirmed with a death rate of 54%. Most cases have occurred within the Arab Peninsula and neighboring countries. Infection with the novel coronavirus has led to severe lower respiratory tract illness. There is a low rate of human-to-human transmission; however, concern has arisen that the virus may adapt to being more efficient at such transmission. 109 RSV is an enveloped RNA virus in the paramyxovirus family, which is primarily associated with fall to winter epidemics of lower respiratory illness in infants and young children. Up to 70% of newborns are infected during their first winter. RSV infection in adults generally represents reinfection, and may be the etiologic agent in up to 2.4% of community-acquired lower respiratory tract infections. 110 Among the elderly, RSV infection is more common and may account for 10% of winter hospital admissions, with a case-fatality rate similar to that of influenza (w10%). 111 Risk factors for severe disease are advanced age, immunocompromised state, and chronic cardiopulmonary diseases, for which higher death rates have been reported. RSV lower respiratory tract infection in adults presents as a wheezing illness in 90% of cases, along with crackles and a pneumonic infiltrate in 40%. However, the classic bronchiolitis picture seen in infants is rare in adult populations. Most adults present with nasal congestion, cough, and low-grade fever, which can be followed by dyspnea and wheezing. Often in adults the clinical features are difficult to distinguish from other respiratory viruses; however, myalgias and fever are less common, and wheezing and rhinorrhea more common, with RSV than with influenza infection. 112 CXR often demonstrates small focal infiltrates, but lobar infiltrates have been described. 92 Diagnosis is best made by RT-PCR of nasal aspirates and, if available, lower respiratory sample (bronchoalveolar lavage or deep tracheal suctioning) or viral cultures, which are less sensitive. The aerosolized form of ribavirin is approved for treatment of RSV in children. Data from adult populations are limited. Ribavirin has been used in immunocompromised adults with upper and lower respiratory tract infections, either alone or in combination with IVIG (standard or RSV-IVIG). 113 Spread is via large droplets and fomites. Isolation and cohorting of infected patients is recommended. Human metapneumovirus (hMPV) is closely related to RSV, and primary infection often occurs in childhood; however, as with RSV, immunity is incomplete. In children the clinical manifestations are very similar to those of RSV. The incidence of symptomatic infection in adults is generally less than 5% in most studies. 114 In a prospective study of hospitalized adults with cardiorespiratory illness during the winter season, hMPV was identified in 8.5% of the cohort. Of these patients, 13% and 12% required ICU admission and ventilatory support, respectively. The mortality rate overall was 7%. Coinfection with RSV, coronavirus, and influenza A was noted in up to 23%. 115 hMPV can result in pneumonia and respiratory failure, although this is less common than with influenza and RSV. 116 The clinical symptoms are indistinguishable from those of other respiratory viruses. Risk factors for severe disease are also similar to those for other viruses and include older age, immunocompromised state, and chronic cardiorespiratory disease. CXR reveals patchy infiltrates, predominantly in the lower lung zones. Identification of the virus optimally involves RT-PCR or direct immunofluorescence, as hMPV replicates very slowly and grows inefficiently using traditional viral culture methods. 114 The mainstay of treatment, as with most viral infections, is supportive. A few case reports and series have reported ribavirin to be a potentially effective treatment, although more studies are needed before this can be recommended. 117 Viruses are an important cause of community-acquired pneumonia in both pediatric and adult populations. Viral pneumonias tend to have a seasonal predilection and are often preceded by a prodromal illness. Disease surveillance systems are important in detecting outbreaks and particularly the emergence of novel viral pathogens capable of human transmission. Several common viral pathogens can lead to severe respiratory disease, including the most common virus, influenza A. Unfortunately, appropriate diagnostic testing is often not pursued or is unavailable, particularly in smaller community hospitals. Treatment of viral pneumonia is generally supportive; however, diagnostic testing to isolate the causative virus is important because some pathogens, such as influenza virus, have effective antiviral therapies. 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