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Pneumonia in US hospitalized patients with influenza-like illness: BioSense, 2007–2010

Published online by Cambridge University Press:  17 July 2012

S. R. BENOIT*
Affiliation:
Division of Notifiable Diseases and Healthcare Information (proposed), Office of Surveillance, Epidemiology, and Laboratory Services, Centers for Disease Control and Prevention (CDC), Atlanta, GA, USA
H. BURKOM
Affiliation:
National Security Technology Department, Johns Hopkins University Applied Physics Laboratory, Laurel, MD, USA
A. F. McINTYRE
Affiliation:
Influenza Division, National Center for Immunization and Respiratory Diseases, CDC, Atlanta, GA, USA
K. KNISS
Affiliation:
Influenza Division, National Center for Immunization and Respiratory Diseases, CDC, Atlanta, GA, USA
L. BRAMMER
Affiliation:
Influenza Division, National Center for Immunization and Respiratory Diseases, CDC, Atlanta, GA, USA
L. FINELLI
Affiliation:
Influenza Division, National Center for Immunization and Respiratory Diseases, CDC, Atlanta, GA, USA
S. JAIN
Affiliation:
Influenza Division, National Center for Immunization and Respiratory Diseases, CDC, Atlanta, GA, USA
*
*Author for correspondence: S. R. Benoit, MD, MPH, CDC, Unit 3190, Box 146, DPO AA 34024-146, USA. (Email: [email protected])
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Summary

We used data from BioSense, a national electronic surveillance system, to describe pneumonia in hospitalized patients with influenza-like illness (ILI). Ninety-five hospitals from 20 states reported ICD-9-CM-coded inpatient final diagnosis data during the study period of September 2007 to February 2010. We compared the characteristics of persons with and without pneumonia among those with ILI-related hospitalizations. BioSense captured 26 987 ILI-related inpatient hospitalizations; 8979 (33%) had a diagnosis of pneumonia. Analysis of trends showed highest counts of pneumonia during the 2007–2008 season and the second 2009 pandemic wave. Pneumonia was more common with increasing age. Microbiology and pharmacy data were available for a subset of patients; 107 (5%) with pneumonia had a bloodstream infection and 17% of patients were prescribed antiviral treatment. Our findings demonstrate the potential utility of electronic healthcare data to track trends in ILI and pneumonia, identify risk factors for disease, identify bacteraemia in patients with pneumonia, and monitor antiviral use.

Type
Original Papers
Creative Commons
This is a work of the U.S. Government and is not subject to copyright protection in the United States.
Copyright
Copyright © Cambridge University Press 2012

INTRODUCTION

Every year in the USA, infection with influenza viruses results in an estimated 86 000–544 000 hospitalizations [Reference Thompson1] and 3349–48 614 deaths [Reference Thompson2]. Persons with underlying medical conditions are at high risk for influenza-associated severe outcomes such as hospitalization and death [3]. Pneumonia is a one of the most common complications of influenza [Reference Dao4, Reference Dawood5]. The characteristics of hospitalized patients with seasonal and pandemic influenza have been described using clinical data obtained through manual medical chart abstraction [Reference Jain6Reference Louie9]. However, to our knowledge, this is the first study to focus on factors associated with pneumonia in hospitalized patients with influenza-like illness (ILI) over multiple influenza seasons using national electronic data.

BioSense is a US national automated surveillance system operated by the Centers for Disease Control and Prevention (CDC) that receives, analyses, and visualizes electronic patient-level healthcare data for public health use [Reference Loonsk10Reference Tokars12]. Data types include chief complaints and final diagnoses from outpatient, emergency department (ED), and inpatient clinical settings; a subset of hospitals send detailed clinical data including microbiology, pharmacy, and radiology information. We used administrative and clinical data from BioSense to (1) track secular trends in ILI and pneumonia, (2) identify risk factors for pneumonia in patients hospitalized with ILI, (3) identify bloodstream infections in patients with ILI and pneumonia, and (4) study the use of influenza antiviral medications in hospitalized ILI patients with and without pneumonia.

METHODS

Study design and case definitions

As of March 2011, over 650 non-federal facilities contributed healthcare data to BioSense. For the purposes of this study, we included only facilities that sent inpatient final diagnosis data consistently over the entire study period (1 September 2007 to 10 February 2010), which reduced the sample size to 95 non-federal facilities in 20 states (Fig. 1).

Fig. 1 [colour online]. Map showing the location of the 95 BioSense study facilities.

This study includes only patients with ILI admitted to the inpatient setting. Chief complaints and diagnosis codes are categorized and assigned to specific sub-syndrome concepts. A hospitalization was classified as ILI-related if its electronic records included a chief complaint and/or final diagnosis of influenza or a combination of BioSense sub-syndromes including fever plus cough or fever plus upper respiratory infection (URI) [13]. We selected this ILI definition because it is used by the majority of US state and local health departments and was adopted by the US Influenza-like Illness Surveillance Network (ILINet) [14, Reference Brammer15]. Furthermore, the positive predictive value of symptoms approximating these criteria has been reported at 79–87% in studies during the influenza season [Reference Monto16, Reference Boivin17]. The definition was validated using BioSense and ILINet data from 2005 to 2008 and produced time-series graphs agreeing in global and local trend behaviour, characterized by mean and median differences below 0·5% [13]. Of patients hospitalized with ILI, we compared those with pneumonia to those without pneumonia, defined by International Classification of Diseases, Ninth Revision, Clinical Modification (ICD-9-CM) final diagnosis codes of 480.x to 486.x and 487·0 which include viral, pneumococcal, other bacterial, and unspecified pneumonia as well as bronchopneumonia and influenza with pneumonia.

Other variables used in the analysis included age group, underlying conditions, and influenza epidemic period. We categorized age as 0–4, 5–17, 18–24, 25–49, 50–64, and ⩾65 years groups which are similar to the age groups used in ILINet [14]. We analysed whether certain underlying conditions considered high risk by the Advisory Committee on Immunization Practices (ACIP) for severe influenza outcomes (asthma, chronic obstructive pulmonary disease (COPD), chronic cardiac disease, diabetes, haemoglobinopathies, immunosuppressive disorders, malignancy, neuromuscular disorders, chronic renal disease, pregnancy, and obesity [3]) were associated with a pneumonia diagnosis in hospitalized ILI patients. The ACIP high-risk underlying conditions were defined based on final diagnosis using ICD-9-CM codes classified by the Agency for Healthcare Research and Quality (AHRQ) Clinical Classification System (CCS) or as described by Mullooly and colleagues [Reference Elixhauser and McCarthy18, Reference Mullooly19]. The CCS categories were used to supplement definitions where more specificity was needed (e.g. asthma instead of chronic pulmonary conditions). Each condition was a separate dichotomous variable.

Influenza epidemic periods were defined as contiguous weeks when ⩾10% of weekly respiratory samples submitted for influenza testing to the national World Health Organization/National Respiratory and Enteric Virus Surveillance System Laboratory Surveillance Network were positive [14]. The 2007–2008 influenza season was from 30 December 2007 to 13 April 2008; the 2008–2009 season from 11 January 2009 to 5 April 2009; the 2009 pandemic H1N1 spring wave from 15 April 2009 to 24 July 2009; and the 2009 pandemic H1N1 autumn wave was from 1 September 2009 to 31 December 2009. The influenza epidemic period was a categorical variable with five levels; ‘no influenza epidemic’ was the reference.

Clinical data

A subset of BioSense facilities sends electronic clinical data (e.g. microbiology, pharmacy). In BioSense, patients are given a unique longitudinal identifier. We used this identifier to link administrative and clinical data associated with a particular hospitalization. For patients with an ICD-9-CM pneumonia diagnosis, we searched the microbiology data for blood culture results by identifying tests with a Logical Observation Identifiers Names and Codes (LOINC) code of 600–7. Most BioSense laboratory data are not Systematized Nomenclature of Medicine-Clinical Terms (SNOMED-CT)-coded, so we used text-parsing methods utilizing Perl regular expressions to identify positive test results [Reference Benoit20]. To avoid identifying contaminant pathogens, we defined a bloodstream infection as a positive blood culture result with one of the following pathogens: Staphylococcus aureus, Steptococcus pneumoniae, beta-haemolytic streptococci, Escherichia coli, Klebsiella pneumoniae, Enterobacter cloacae, Serratia marcescens, Proteus mirabilis, Pseudomonas aeruginosa, Bacteroides spp., and Candida spp. [Reference Pien21].

After identifying pneumonia patients with bloodstream infections, we stratified by influenza epidemic period and characterized the patients based on pathogen, age group, underlying conditions, and disposition. A patient was considered to have a hospital-onset bloodstream infection if the specimen yielding the positive result was collected on or after the fourth day of hospitalization (where the date of hospitalization was day 1) [Reference Kallen22]. An infection was defined as community-onset, hospital associated if a positive specimen was collected before the fourth day of hospitalization and the patient had been hospitalized overnight at least once in the same healthcare system ⩽30 days before the date of specimen collection [Reference Benoit20]. Otherwise, the patient was considered to have a community-onset infection which included patients whose infection onset was in the community and who had either no hospitalizations in the previous 30 days or who had a hospitalization in a healthcare system not captured by the BioSense system.

Inpatient pharmacy data were used to assess the proportion of patients receiving an influenza antiviral medication (oseltamivir or zanamivir) during their hospitalization, stratifying by influenza epidemic period and pneumonia diagnosis. We used text parsing methods and searched for brand names in addition to the generic-named oseltamivir and zanamivir. Only patients with at least one medication on record were included in the analysis.

Data analysis

We describe the population of hospitalized ILI patients by pneumonia status stratified by age group, underlying disease, and influenza epidemic period. Differences between those with and without pneumonia were assessed using the χ2 test. ILI, ILI + pneumonia, and pneumonia (no ILI) visit counts were displayed with a time-series plot. Logistic regression was used to investigate the association of a pneumonia diagnosis with underlying conditions while controlling for influenza epidemic periods. A preliminary model showed significant interaction terms between age groups and some underlying medical conditions. Therefore, separate multivariable models were created for four age groups; i.e. 0–4 and 5–17 years age groups as well as the 18–24 and 25–49 years age groups were combined so that the sample sizes within each category were adequate for analysis. All applicable underlying conditions were included in the models because many patients had multiple conditions. A separate model was run to test the association of pregnancy and pneumonia in females in the 18–49 years age group while controlling for underlying conditions and influenza epidemic periods. Goodness of fit of each model was assessed with the Hosmer–Lemeshow test. Statistical analyses were conducted using SAS 9.2 (SAS Institute Inc., USA).

RESULTS

Characteristics of study patients

From 1 September 2007 to 10 February 2010, BioSense captured 26 987 inpatient hospitalizations with ILI from 26 000 unique patients; 8979 (33%) hospitalizations (8794 unique patients) had an ICD-9-CM diagnosis of pneumonia. Figure 2 displays weekly counts of ILI, ILI + pneumonia, and pneumonia (no ILI) hospitalizations; in general, the two ILI curves trend together. The pneumonia-only curve shows more gradual rises during the winter months. The 2009 rise in the ILI and ILI + pneumonia curves occur early relative to the usual influenza season and out of proportion to the usual number of visits. While ILI and ILI + pneumonia visits start to fall in December of 2009, the pneumonia-only visits continue to rise. The four influenza epidemic periods totalled 58 weeks compared to 71 non-epidemic weeks, yet 65% of the pneumonia-with-ILI diagnoses occurred during the influenza epidemic periods (Tables 1 and 2). The number of pneumonia admissions per week peaked during the 2009 pandemic H1N1 autumn season (147 per week compared to 44 per week during non-epidemic periods, relative risk 3·4) and was highest in the 25–49 years age group (41 compared to nine per week) (Table 1).

Fig. 2 [colour online]. Hospitalized patients with influenza-like illness (ILI) and ILI + pneumonia, BioSense (1 September 2007 to 10 February 2010). (a) 2007–2008 seasonal H3N2 period (30 December 2007 to 13 April 2008); (b) 2008–2009 seasonal H1N1 (11 January 2009 to 5 April 2009); (c) 2009 pandemic H1N1 spring wave (15 April 2009 to 24 July 2009); (d) 2009 pandemic H1N1 autumn wave (1 September 2009 to 31 December 2009).

Table 1. Pneumonia diagnosis per week and pneumonia diagnosis counts stratified by age group and influenza epidemic period for hospitalized patients with influenza-like illness, BioSense, 1 September 2007 to 10 February 2010

n.a., Not applicable.

* Influenza seasons: 2007–2008 influenza season (from 30 December 2007 to 13 April 2008); 2008–2009 season (from 11 January 2009 to 5 April 2009); 2009 pandemic H1N1 spring wave (from 15 April 2009 to 24 July 2009); and the 2009 pandemic H1N1 autumn wave (from 1 September 2009 to 31 December 2009).

0–4 years is the reference.

The number of pneumonia diagnoses for the corresponding influenza epidemic period and age group divided by the number of weeks for that epidemic period.

Table 2. Characteristics of hospitalized patients with influenza-like illness stratified by pneumonia diagnosis, BioSense, 1 September 2007 to 10 February 2010

COPD, Chronic obstructive pulmonary disease.

* Influenza seasons: 2007–2008 (from 30 December 2007 to 13 April 2008); 2008–2009 (from 11 January 2009 to 5 April 2009); 2009 pandemic H1N1 spring wave (from 15 April 2009 to 24 July 2009); and 2009 pandemic H1N1 autumn wave (from 1 September 2009 to 31 December 2009).

Sample is restricted to females aged 18–49 years, denominator for those with pneumonia and no pneumonia was 1296 and 2957, respectively.

The age distribution of hospitalizations with ILI and pneumonia was different than those with ILI alone (P < 0·001, Table 2). A greater proportion of hospitalizations with ILI and pneumonia occurred among those aged ⩾65 years. The relative risk of pneumonia increased from 1·0 in the 0–4 years age group to 1·8 in the ⩾65 years age group (Table 1). Additionally, the proportion of ILI hospitalizations that occurred during the 2009 pandemic H1N1 autumn wave was higher for those with pneumonia (28%) than the corresponding proportion without pneumonia (24%). With the exception of haemoglobinopathies and pregnancy, the prevalence of underlying conditions was significantly higher in hospitalized ILI patients with vs. those without pneumonia (P < 0·001) (Table 2).

Logistic regression models were constructed separately for each of four age groups, including indicator variables for underlying conditions while controlling for influenza epidemic period. The Hosmer–Lemeshow goodness-of-fit test for similarity of predicted/observed values by decile gave P values from 0·6 to 0·9 except for the 50–64 years age group where the P value was still acceptable at 0·09. In the 0–17 years age group, neuromuscular disease [odds ratio (OR) 1·9] and asthma (OR 1·7) were associated with pneumonia after controlling for influenza epidemic period and all other underlying conditions (Table 3). In the older age groups, COPD (OR 1·2–2·1) and immunosuppressive disorder (OR 1·4–1·5) were consistently associated with pneumonia. In the 18–49 years age group, the odds of pneumonia was 1·3 times higher in obese patients, and pregnancy (OR 0·4) was protective for pneumonia.

Table 3. Underlying conditions associated with a pneumonia diagnosis stratified by age group and controlling for influenza epidemic period* in hospitalized patients with influenza-like illness, BioSense, 1 September 2007 to 10 February 2010

OR, Odds ratio; CI, confidence interval; COPD, Chronic obstructive pulmonary disease; n.a., not applicable.

* Influenza seasons: 2007–2008 influenza season (from 30 December 2007 to 13 April 2008); 2008–2009 (from 11 January 2009 to 5 April 2009); 2009 pandemic H1N1 spring wave (from 15 April 2009 to 24 July 2009); and 2009 pandemic H1N1 autumn wave (from 1 September 2009 to 31 December 2009).

Multivariable odds ratio.

This variable was not included in the multivariable model; a separate model was run with this variable only plus influenza epidemic period.

Bold values are statistically significant at an alpha level of 0·05.

Clinical data

Blood culture data were available for 2212 (25%) hospitalizations with a pneumonia diagnosis, and of those, 107 (5%) patients had a bloodstream infection (110 pathogens), including 2% of children aged <18 years and 5% of adults aged ⩾18 years. The most commonly identified pathogen was S. pneumoniae (37%) followed by S. aureus (22%). Of the 107 patients with bloodstream infection, the median age was 52 years [interquartile range (IQR) 35–61 years]. Eighty-eight (82%) of the patients had at least one ACIP high-risk underlying condition with the most common being cardiac disease (49%). Forty (37%) of the 107 patients were hospitalized during the 2009 pandemic H1N1 autumn epidemic period, equating to 2·4 hospitalizations with bloodstream infections per week compared to 0·5 per week during non-influenza epidemic periods. The majority (63%) of bloodstream infections was community-onset; 26% were hospital-onset and 11% were community-onset, hospital associated. Of the hospital-onset infections, the most commonly identified pathogens were Candida spp. (n = 8), S. aureus (n = 6), K. pneumoniae (n = 5), and E. coli (n = 5). Seventeen (16%) of the 107 patients with a bloodstream infection died; of those, 10 (59%) infections were hospital-onset, the median age of patients was 55 years (IQR 47–66 years), and the most commonly identified pathogen was Candida spp. (n = 5).

Pharmacy data were available for about 48% of the study hospitalizations (n = 11 947). Overall, 17% of study patients received influenza antiviral treatment, including 10% of children aged <18 years and 19% of adults aged ⩾18 years. Except for the 2008–2009 seasonal influenza period, use of influenza antiviral treatment was higher during influenza epidemic periods than during non-epidemic periods, regardless of pneumonia status (Table 4). This epidemic-associated influenza antiviral use increase was especially true during the 2009 pandemic H1N1 autumn period when 55% of those with pneumonia were treated with an antiviral vs. 9% during non-epidemic periods (37% vs. 3% for those without pneumonia). Overall, antiviral treatment was more common in those with pneumonia (23%) than those without pneumonia (14%) (χ2, P < 0·0001). These proportions were higher when limiting the ILI hospitalizations to just those with an influenza ICD-9-CM diagnosis code; 44% with pneumonia vs. 28% without pneumonia received an influenza antiviral (not shown in Table 4, P < 0·0001).

Table 4. Antiviral treatment* for hospitalized patients with influenza-like illness stratified by influenza epidemic period and pneumonia status, BioSense, 1 September 2007 to 10 February 2010

* Oseltamivir or zanamivir.

Influenza seasons: 2007–2008 influenza season (from 30 December 2007 to 13 April 2008); 2008–2009 season (from 11 January 2009 to 5 April 2009); 2009 pandemic H1N1 spring wave (from 15 April 2009 to 24 July 2009); and 2009 pandemic H1N1 autumn wave (from 1 September 2009 to 31 December 2009).

DISCUSSION

We analysed administrative and clinical data from 26 000 hospitalized patients with ILI reported to BioSense from 1 September 2007 to 10 February 2010 to evaluate characteristics associated with a pneumonia diagnosis. Hospitalized patients with ILI and ILI + pneumonia followed a similar pattern with the 2007–2008 influenza season and 2009 pandemic H1N1 autumn wave being more severe than the 2008–2009 season. Overall, hospitalized patients with ILI and a pneumonia diagnosis compared to those without pneumonia were older and had a higher proportion of underlying conditions. Almost 5% of pneumonia patients had a bloodstream infection and patients with pneumonia were more likely to be treated with influenza antiviral agents, especially during influenza epidemic periods. These data correlate well with published studies using primary data collection of seasonal [Reference Dao4, Reference Dawood5] and pandemic [Reference Jain6, Reference Skarbinski7] influenza hospitalizations, including influenza-associated pneumonia [Reference Dawood5]. To our knowledge, this is the first study in the USA to use strictly electronic healthcare data to describe ILI and pneumonia over multiple influenza seasons including the pandemic influenza season of 2009–2010.

Administrative healthcare data such as final diagnosis codes are a low cost, readily available means of obtaining a broad picture of clinical events and trends without the challenges of primary data collection. The magnitude and volume of these data potentially outweigh their imperfections. Furthermore, these data allow a quantitative grasp of the burden of disease that can be compared across years and cannot be achieved with small, time-limited and expensive clinical studies. For example, the number of hospitalizations with ILI and a pneumonia diagnosis per week was higher during the 2007–2008 seasonal epidemic than during non-influenza epidemic periods by an overall factor of 2·4 (104·2 vs. 43·7) (Table 1, Fig. 2). However, that factor varied by age group and was 3·2 for the ⩾65 year age group, 2·0 for patients aged <5 years, and 1·6 for other patients aged <25 years. By contrast, the 2009 pandemic H1N1 autumn wave saw an overall pneumonia increase factor of 3·4, clearly a greater burden overall, with more than fourfold increases for age groups from 5–44 years and with the largest factor increase of 5·4 in the 5–17 years group. The morbidity seen in the younger age groups during the 2009 pandemic H1N1 autumn wave was in contrast to previous trends. From 1979 to 2001, Thompson et al. [Reference Thompson1] demonstrated increasing pneumonia and influenza hospitalization rates in older age groups using representative discharge diagnosis data. BioSense data, available in near real-time, can identify changes in these patterns of disease.

The US healthcare sector is now focused on the ‘meaningful use’ of electronic health records (EHR), a Department of Health and Human Services legislation incentivizing healthcare providers and institutions to adopt EHR. Given the movement towards EHR implementation, it is reassuring that our study correlated well with current surveillance data and published literature on influenza and pneumonia. We found the trend in pneumonia among hospitalized ILI patients increased by age group; a finding consistent with national hospital discharge data [Reference Hall23]. During influenza epidemic periods, the proportion of pneumonia in hospitalized adults (⩾18 years) and children (<18 years) with ILI in BioSense was 38% and 25%, respectively. Our results are similar to findings from a large multi-site influenza hospitalizations surveillance system in which among patients hospitalized with laboratory-confirmed influenza over multiple non-pandemic influenza seasons, 34% of adults and 36% of children had evidence of pneumonia [Reference Dao4, Reference Dawood5] (Table 5).

Table 5. Pneumonia, bloodstream infection, and antiviral data from BioSense compared to other studies

* Includes all sterile sites (blood, cerebrospinal fluid, pleural fluid, and tissue specimen).

Includes only 2007–2008 data and patients with a final diagnosis code of influenza to attempt to match time period and methods of Dawood et al. [Reference Dawood5].

Includes only 2009 pandemic H1N1 spring and autumn waves and patients with a final diagnosis code of influenza to attempt to match time period and methods of Jain et al. [Reference Jain6] and Skarbinski et al. [Reference Skarbinski7]

§ Includes only 2007–2008 data and patients with a final diagnosis code of influenza to attempt to match time period and methods of Dao et al. [Reference Dao4].

Includes only patients with a final diagnosis code of influenza.

The majority of patients hospitalized with ILI and pneumonia had underlying medical conditions. Although there are no comparable data sources that evaluate the prevalence of underlying conditions in hospitalized patients with ILI, our findings are consistent with published studies of laboratory-confirmed influenza hospitalizations which also report that a large proportion of both children [Reference Dawood5] and adults [Reference Dao4] hospitalized with influenza have underlying medical conditions. In children, similar to our study, underlying conditions of asthma and neuromuscular disease have been significantly associated with influenza-related pneumonia while haemoglobinopathies were protective [Reference Dawood5]. Dawood et al. [Reference Dawood5] gave the explanation that the protective effect of haemoglobinopathy relative to pneumonia may result from a lower threshold for hospitalization due to this chronic condition in children [Reference Dawood5]. We also found a protective effect of pregnancy with pneumonia. The same explanation may apply to this association.

Overall, we found that almost 5% of the ILI-hospitalized patients with pneumonia also had a bloodstream infection; the event rate for bloodstream infections was 2·5-fold higher during influenza epidemic periods than non-epidemic periods. In children, this proportion was lower (2·4%), similar to the result of Dawood et al. (2·0%) [Reference Dawood5] (Table 5). In contrast to other studies [Reference Dao4, Reference Dawood5] where S. aureus was the predominant pathogen in invasive infections, we found S. pneumoniae most commonly identified. The relationship between influenza, with and without pneumonia, and bacterial co-infections has been well described [Reference Brundage24]. Possible mechanisms for influenza and bacterial co-infection include the destruction of the epithelial cell layer of the tracheobronchial tree by the influenza virus [Reference Hers, Masurel and Mulder25, Reference Peltola and McCullers26] and influenza virus-induced immunosuppression [Reference Peltola and McCullers26Reference Jakab28], both of which would allow for vulnerability to acquire a bacterial infection. The strong association between ILI and pneumonia during influenza epidemic periods in our study supports the described biological mechanisms but we can not infer causation using our data.

This is the first study to correlate clinical information about ILI and pneumonia to the receipt of antiviral agents for the treatment of influenza. Of 9035 ILI hospitalizations with pharmacy data for adults and 2912 for children, 19% and 10%, respectively, were treated with oseltamivir or zanamivir. These proportions were higher in adults (25%) and children (16%) when restricting the sample to those with ILI and pneumonia. Compared to previous seasons, there was a marked increase in influenza antiviral use from 3% to 14% during the 2007–2009 season to 36% during the 2009 pandemic H1N1 season which is in accordance with CDC guidelines and findings from other observational studies [Reference Skarbinski7, Reference Belongia8, 29, Reference Doshi30]. During the 2003–2008 influenza seasons, Dawood et al. found that 20% of children hospitalized with laboratory-confirmed influenza who had pneumonia were treated with antivirals [Reference Dawood5]. For BioSense hospitalizations restricted to the 2007–2008 season and including only those with a final diagnosis of influenza in order to attempt to best match time period and diagnostic precision of the Dawood et al. [Reference Dawood5] study, 22% of children received antivirals (Table 5). The antiviral treatment proportions in our study (14% in the 2009 pandemic H1N1 spring and 44% in the autumn wave) were lower compared to ⩾75% in Jain et al. [Reference Jain6] and Skarbinski et al. [Reference Skarbinski7], perhaps because BioSense receives only inpatient pharmacy data and some patients may have received treatment prior to hospitalization. Further, our data are based on ILI rather than laboratory-confirmed influenza. When restricting the sample to patients with a final diagnosis of influenza, the proportions receiving influenza antiviral treatment rose (Table 5). Finally, the completeness of BioSense pharmacy data is also unknown. However, it is plausible that patients in our study, especially those without laboratory-confirmed influenza, may not have received influenza antivirals, suggesting the underutilization of influenza antivirals. CDC and ACIP guidelines state the importance of early and aggressive antiviral treatment in all hospitalized patients when influenza is suspected, even if testing is not done [Reference Fiore31].

This study was subject to several limitations. First, our ILI definition may have caused under-ascertainment of influenza in the elderly who are less likely to mount a fever. However, even if fever was not present, elderly patients would be captured with an ICD-9-CM code for influenza or a chief complaint of ILI or influenza. BioSense facilities are not representative of all U.S. hospitals; they are a convenience sample of facilities that are able and willing to send electronic healthcare data. Additionally, only a subset of the facilities sent microbiology and pharmacy data so we were unable to link these clinical data types for all hospitalizations. ICD-9-CM codes are not confirmatory for underlying conditions or pneumonia and we did not validate these diagnoses with hospital chart abstraction. Similarly, completeness or accuracy of electronic healthcare data was not verified by chart abstraction. Pneumonia can be attributed to multiple factors which were not accounted for in this study. Pneumococcal vaccination, for example, was not available in BioSense data and whether the magnitude or direction of the multivariable model findings would change with the inclusion of other factors is unknown. Finally, our study was based on a syndromic ILI definition using either patient chief complaint or ICD-9-CM final diagnosis codes. However, depending on the codes used, the correlation between laboratory-based and syndromic influenza detection is as high as 0·86 (P < 0·0001), suggesting syndromic-based detection may be a useful approach [Reference Marsden-Haug32].

Our study also has several strengths. As pointed out above, some of our findings are markedly consistent with data from laboratory-confirmed influenza hospitalizations surveillance and these data add insights into epidemic trends. Overall, the volume of BioSense's electronic data may facilitate study of selected issues which are less affected by its limitations. Our study of 26 000 unique ILI patients from 95 facilities in 20 states would not have been feasible with medical chart abstraction. Electronic systems require start-up costs, but, once established, provide timely data without burdening healthcare personnel with manual data abstraction.

This study is the first to explore ILI-related pneumonia in hospitalized patients using exclusively electronic administrative and clinical data. The clinical data, although only available for a subset of the hospitalizations, supplement the diagnosis codes with a richer characterization of the disease and treatment course without any additional burden on data collection. Although these data are not derived from an EHR, these are the types of data that will become available as ‘meaningful use’ compliant EHRs become more widely available. This study provides an example of how electronic data can be used to track ILI and pneumonia disease trends, explore risk factors for disease, identify bloodstream infections using microbiology data, and study influenza antiviral prescribing patterns.

ACKNOWLEDGEMENTS

We thank Jerome I. Tokars for his contributions in the review of this manuscript. The findings and conclusions in this report are those of the authors and do not necessarily represent the official position of the Centers for Disease Control and Prevention.

DECLARATION OF INTEREST

None.

References

REFERENCES

1.Thompson, WW, et al. Influenza-associated hospitalizations in the United States. Journal of the American Medical Association 2004; 292: 13331340.CrossRefGoogle ScholarPubMed
2.Thompson, MG, et al. Estimates of deaths associated with seasonal influenza – United States, 1976–2007. Morbidity and Mortality Weekly Report 2010; 59: 10571062.Google Scholar
3.Centers for Disease Control and Prevention. Prevention and Control of Influenza with Vaccines: Recommendations of the Advisory Committee on Immunization Practices (ACIP), 2010. Morbidity and Mortality Weekly Report 2010; 59: 162.Google Scholar
4.Dao, CN, et al. Adult hospitalizations for laboratory-positive influenza during the 2005–2006 through 2007–2008 seasons in the United States. Journal of Infectious Diseases 2010; 202: 881888.CrossRefGoogle ScholarPubMed
5.Dawood, FS, et al. Influenza-associated pneumonia in children hospitalized with laboratory-confirmed influenza, 2003–2008. Pediatric Infectious Disease Journal 2010; 29: 585590.CrossRefGoogle ScholarPubMed
6.Jain, S, et al. Hospitalized patients with 2009 H1N1 influenza in the United States, April-June 2009. New England Journal of Medicine 2009; 361: 19351944.CrossRefGoogle ScholarPubMed
7.Skarbinski, J, et al. Hospitalized patients with 2009 pandemic influenza A (H1N1) virus infection in the United States – September–October 2009. Clinical Infectious Diseases 2011; 52: S50S59.CrossRefGoogle ScholarPubMed
8.Belongia, EA, et al. Clinical characteristics and 30-day outcomes for influenza A 2009 (H1N1), 2008–2009 (H1N1), and 2007–2008 (H3N2) infections. Journal of the American Medical Association 2010; 304: 10911098.CrossRefGoogle ScholarPubMed
9.Louie, JK, et al. Factors associated with death or hospitalization due to pandemic 2009 influenza A(H1N1) infection in California. Journal of the American Medical Association 2009; 302: 18961902.CrossRefGoogle ScholarPubMed
10.Loonsk, JW. BioSense – a national initiative for early detection and quantification of public health emergencies. Morbidity and Mortality Weekly Report 2004; 53: 5355.Google Scholar
11.Bradley, CA, et al. BioSense: implementation of a National Early Event Detection and Situational Awareness System. Morbidity and Mortality Weekly Report 2005; 54: 1119.Google ScholarPubMed
12.Tokars, JI, et al. Summary of data reported to CDC's national automated biosurveillance system, 2008. BioMed Central Medical Informatics and Decision Making 2010; 10: 30.CrossRefGoogle ScholarPubMed
13.The BioSense Influenza Module (http://www.syndromic.org/conference/2008/presentations/powerpoints.htm). Accessed 16 June 2011.Google Scholar
14.Centers for Disease Control and Prevention (http://www.cdc.gov/flu/weekly/overview.htm). Accessed 20 March 2011.Google Scholar
15.Brammer, L, et al. Surveillance for influenza during the 2009 influenza A (H1N1) pandemic-United States, April 2009-March 2010. Clinical Infectious Diseases 2011; 52: S27S35.CrossRefGoogle ScholarPubMed
16.Monto, AS, et al. Clinical signs and symptoms predicting influenza infection. Archives of Internal Medicine 2000; 160: 32433247.CrossRefGoogle ScholarPubMed
17.Boivin, G, et al. Predicting influenza infections during epidemics with use of a clinical case definition. Clinical Infectious Diseases 2000; 31: 11661169.CrossRefGoogle ScholarPubMed
18.Elixhauser, A, McCarthy, EM.Clinical classifications for health policy research, version 2: Hospital inpatient statistics. Healthcare Cost and Utilization Project (HCUP 3) Research Note 1. Rockville, MD: Agency for Health Care Policy and Research, 1996; AHCPR Pub. No. 96 0017 (http://www.hcup-us.ahrq.gov/toolssoftware/ccs/ccs.jsp). Accessed 10 March 2011.Google Scholar
19.Mullooly, JP, et al. Influenza- and RSV-associated hospitalizations among adults. Vaccine 2007; 25: 846855.CrossRefGoogle ScholarPubMed
20.Benoit, SR, et al. Automated surveillance of Clostridium difficile infections using BioSense. Infection Control and Hospital Epidemiology 2011; 32: 2633.CrossRefGoogle ScholarPubMed
21.Pien, BC, et al. The clinical and prognostic importance of positive blood cultures in adults. American Journal of Medicine 2010; 123: 819828.CrossRefGoogle ScholarPubMed
22.Kallen, AJ, et al. Health care-associated invasive MRSA infections, 2005–2008. Journal of the American Medical Association 2010; 304: 641648.CrossRefGoogle ScholarPubMed
23.Hall, MJ, et al. National Hospital Discharge Survey: 2007 Summary. National health statistics reports; no. 29. Hyattsville, MD: National Center for Health Statistics, 2010.Google Scholar
24.Brundage, JF. Interactions between influenza and bacterial respiratory pathogens: implications for pandemic preparedness. Lancet Infectious Diseases 2006; 6: 303312.CrossRefGoogle ScholarPubMed
25.Hers, JF, Masurel, N, Mulder, J. Bacteriology and histopathology of the respiratory tract and lungs in fatal Asian influenza. Lancet 1958; 2: 11411143.CrossRefGoogle ScholarPubMed
26.Peltola, VT, McCullers, JA. Respiratory viruses predisposing to bacterial infections: role of neuraminidase. Pediatric Infectious Disease Journal 2004; 23: S87S97.CrossRefGoogle ScholarPubMed
27.Nickerson, CL, Jakab, GJ. Pulmonary antibacterial defenses during mild and severe influenza virus infection. Infection and Immunity 1990; 58: 28092814.CrossRefGoogle ScholarPubMed
28.Jakab, GJ. Immune impairment of alveolar macrophage phagocytosis during influenza virus pneumonia. American Review of Respiratory Disease 1982; 126: 778782.Google ScholarPubMed
29.Centers for Disease Control and Prevention (http://www.cdc.gov/H1N1flu/recommendations.htm#c). Accessed 2 May 2011.Google Scholar
30.Doshi, S, et al. Comparison of antiviral treatment among hospitalized adults before and during the 2009 influenza pandemic – United States, 2005–09. Proceedings of the 48th Annual Meeting of the IDSA. 21–24 October, 2010. Vancouver, Canada: Infectious Diseases Society of America, 2010.CrossRefGoogle Scholar
31.Fiore, AE, et al. Antiviral agents for the treatment and chemoprophylaxis of influenza – recommendations of the Advisory Committee on Immunization Practices (ACIP). Morbidity and Mortality Weekly Report 2011; 60: 124.Google ScholarPubMed
32.Marsden-Haug, N, et al. Code-based syndromic surveillance for influenza-like illness by International Classification of Diseases, Ninth Revision. Emerging Infectious Diseases 2007; 13: 207216.CrossRefGoogle Scholar
Figure 0

Fig. 1 [colour online]. Map showing the location of the 95 BioSense study facilities.

Figure 1

Fig. 2 [colour online]. Hospitalized patients with influenza-like illness (ILI) and ILI + pneumonia, BioSense (1 September 2007 to 10 February 2010). (a) 2007–2008 seasonal H3N2 period (30 December 2007 to 13 April 2008); (b) 2008–2009 seasonal H1N1 (11 January 2009 to 5 April 2009); (c) 2009 pandemic H1N1 spring wave (15 April 2009 to 24 July 2009); (d) 2009 pandemic H1N1 autumn wave (1 September 2009 to 31 December 2009).

Figure 2

Table 1. Pneumonia diagnosis per week and pneumonia diagnosis counts stratified by age group and influenza epidemic period for hospitalized patients with influenza-like illness, BioSense, 1 September 2007 to 10 February 2010

Figure 3

Table 2. Characteristics of hospitalized patients with influenza-like illness stratified by pneumonia diagnosis, BioSense, 1 September 2007 to 10 February 2010

Figure 4

Table 3. Underlying conditions associated with a pneumonia diagnosis stratified by age group and controlling for influenza epidemic period* in hospitalized patients with influenza-like illness, BioSense, 1 September 2007 to 10 February 2010

Figure 5

Table 4. Antiviral treatment* for hospitalized patients with influenza-like illness stratified by influenza epidemic period† and pneumonia status, BioSense, 1 September 2007 to 10 February 2010

Figure 6

Table 5. Pneumonia, bloodstream infection, and antiviral data from BioSense compared to other studies