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Original research
Incidence, aetiology and serotype coverage for pneumococcal vaccines of community-acquired pneumonia in adults: a population-based prospective active surveillance study in Brazil
  1. Fernanda Gross Duarte1,
  2. Maria Goreth Barberino1,
  3. Sandra da Silva Moreira2,
  4. Joice Neves Reis3,
  5. Julia Regazzini Spinardi4,
  6. Rodrigo Sini de Almeida5,
  7. Kristen E Allen6,
  8. Ronika Alexander-Parrish6,
  9. Rosa Brim3,
  10. César Augusto de Araújo Neto3,
  11. Edson Duarte Moreira1,2
  1. 1Gonçalo Moniz Institute, Oswaldo Cruz Foundation, Brazilian Ministry of Health, Salvador, Bahia, Brazil
  2. 2Centro de Pesquisa Clínica (CPEC), Obras Sociais Irma Dulce, Salvador, Bahia, Brazil
  3. 3Federal University of Bahia, Salvador, Brazil
  4. 4Pfizer Brasil, Sao Paulo, Brazil
  5. 5Pfizer Inc, New York, New York, USA
  6. 6Pfizer Inc Pennsylvania, Collegeville, Pennsylvania, USA
  1. Correspondence to Jr. Edson Duarte Moreira; edson.moreira{at}fiocruz.br

Abstract

Objectives To determine the incidence, aetiology and pneumococcal serotype distribution of community-acquired pneumonia (CAP) in Brazilian adults during a 2-year period.

Design Prospective population-based surveillance study.

Setting Patients from two emergency hospitals in Brazil were consecutively included in this study.

Participants A total of 111 adults aged 50 years and older with radiographically-confirmed CAP requiring an emergency department visit were prospectively enrolled between January 2018 and January 2020.

Main outcome measures Incidence rates of CAP were calculated according to age and pathogen. Pathogens were identified by conventional microbiological methods. Additionally, a novel, Luminex-based serotype specific urinary antigen detection assay was used to detect serotypes included in pneumococcal vaccines.

Results Mean age of participants was 64 years and 31% were aged ≥70 years. Aetiology was established in 61 (57%) patients; among identified cases, the most common pathogens were Streptococcus pneumoniae (42/61, 69%) and influenza (4/61, 7%). Among serotypes identified from the 42 cases of pneumococcal CAP, estimated coverage ranged by pneumococcal vaccine formulations from 47.6% (13-valent), 59.5% (20-valent, licenced in the USA only) and 71.4% (23-valent). In patients with CAP, 20-valent pneumococcal vaccine serotypes were identified 2.5 times more frequently than 10-valent pneumococcal vaccine serotypes (22.5% vs 9.0%). The incidence rate for CAP in adults aged ≥50 years was 20.1 per 10 000 person-years. In general, the incidence of CAP increased consistently with age, reaching 54.4 (95% CI 36.8 to −76.6) per 10 000 in adults 80 years or older.

Conclusions We observed a high burden of pneumococcal CAP among adults in Brazil. Despite the routine immunisation of children and high-risk adults against pneumococcal disease in the Brazilian national vaccination programme, a persistent burden of pneumococcal CAP caused by vaccine serotypes remains in this population.

  • Community-acquired pneumonia
  • Incidence
  • Pneumococcal vaccines
  • Streptococcus pneumoniae
  • Serotype distribution

Data availability statement

Data are available upon reasonable request.

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This is an open access article distributed in accordance with the Creative Commons Attribution Non Commercial (CC BY-NC 4.0) license, which permits others to distribute, remix, adapt, build upon this work non-commercially, and license their derivative works on different terms, provided the original work is properly cited, appropriate credit is given, any changes made indicated, and the use is non-commercial. See: http://creativecommons.org/licenses/by-nc/4.0/.

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Strengths and limitations of this study

  • Prospective, population-based active surveillance study aimed to estimate incidence rate of community-acquired pneumonia (CAP) in adults, conducted over a period of two consecutive years.

  • All cases of CAP were radiographically confirmed and validated by clinical information.

  • Non-cultured-based tests employed to improve the detection of Streptococcus pneumoniae in non-bacteraemic cases of CAP.

  • Some patients with mild symptoms may have been missed because they did not seek an emergency department for evaluation.

  • A thorough virological research was not performed.

Introduction

Community-acquired pneumonia (CAP) is associated with substantial morbidity and mortality, accounting for more than 290 million cases and 4.9% of all deaths in the world.1 Pneumonia kills more children worldwide than any other infectious disease, claiming the lives of over 800 000 children under 5 years of age every year, or around 2200 every day.2 In Brazil, CAP is the third cause of mortality and the leading infectious cause of hospital admission and death among adults, with 598 668 CAP-related hospitalisations and 52 776 CAP-related deaths in 2017.3 4 Therefore, CAP is a global public health problem, responsible for a considerable burden and the utilisation of healthcare resources in all age groups.

The incidence of CAP varies by age, being higher in children and older adults.5 It also varies by region—estimates of annual incidences from studies conducted in community-dwelling adults aged ≥18 years living in Latin America range from 1.8 to 7.0 per 1000 person-years,6 whereas it ranges from 2.5 to 6.5 in patients hospitalised with CAP per 1000 adults in the USA, 2.5–11.6 cases per 1000 from selected countries in Europe.7–10 Various pathogens can cause CAP, including both bacteria and viruses, but in as many as half of cases an aetiological agent cannot be identified.8 Streptococcus pneumoniae has been the most commonly identified bacteria implicated in CAP in adults8 11; however, its contribution in the aetiology of CAP differs according to reports that may reflect differences in study design, laboratory isolation of S. pneumoniae and the difficulty with detection of S. pneumoniae in non-bacteraemic CAP.

Limited data are available regarding the incidence of CAP in Brazil. Most estimates were made before the routine administration of the pneumococcal conjugate vaccine in children or in adults at increased risk for pneumococcal disease. Moreover, previous studies included only children12 or were mostly retrospective and have not used more sensitive antigen-based laboratory diagnostic tests.5 13 Routine childhood immunisation with 10-valent pneumococcal conjugated vaccine (PCV10) in Brazil begun in 2010, averaging a vaccination coverage of 85.5%.14 The 13-valent pneumococcal conjugated vaccine (PCV13) and the 23-valent pneumococcal polysaccharide vaccine (PPV23) have been available on the National Immunization Program since 2019, but only for children and adults at higher risk of developing a pneumococcal infection.15 A national passive surveillance system in place, shows that disease by PCV10 serotypes are declining in children, but non-PCV10 serotypes, specially PCV13 exclusive serotypes represent an important proportion of the remaining disease burden in all age groups, including the elderly.16 17 Since most of the pneumococcal disease burden are clinically presented as CAP, additional active surveillance studies are needed to determine the incidence and aetiology of CAP in Brazilian adults.

Advanced age is associated not only with a higher incidence of CAP but also with more severe disease, greater need for hospitalisation and higher mortality.18 Thus, we conducted an active, population-based surveillance study of patients with CAP requiring an emergency department visit among adults 50 years and older in Brazil. We used conventional bacteriological testing and more sensitive non-culture-based methods to determine the incidence and microbiological causes of CAP. In addition to information about disease burden, data on the serotype distribution of pneumococcal strains causing pneumonia in adults were presented.

Methods

Study design and setting

This was a prospective, multicentre, population-based, active surveillance study to identify CAP cases among adults requiring an emergency department visit. Radiographically-confirmed CAP was further assessed by conventional and non-culture-based identification methods. The study was conducted over a period of 24 consecutive months, from 3 January 2018 to 2 January 2020, at two emergency hospitals (Unidade de Pronto Atendimento (UPA)-Barris and UPA-Brotas), in the city of Salvador, Brazil. These study sites serve the public sector of the Brazilian health system, the ‘Sistema Único de Saúde’ (SUS), and are considered public hospitals. The hospitals were selected based on an objective review of site capability to conduct the active surveillance, capacity to enrol patients, ability to collect and test specimens and availability of denominator data for incidence calculations. Weekly study-site visits, enrolment reports and data audits were conducted to ensure standardised procedures in both study sites.

Study population

We sought to enrol all eligible adults 50 years of age or older. Trained nurses screened adults for enrolment at least 18 hours per day, 7 days per week. Screening was conducted in all patients attending the emergency department who presented with evidence of an acute respiratory illness or infection with at least two of the following: fever (axillar temperature ≥38.0°C), hypothermia (axillar temperature <35.5°C, measured by a healthcare provider), chills or rigours, pleuritic chest pain, new or worsening cough, purulent sputum or changes in sputum characteristics, dyspnoea (shortness of breath) or tachypnoea (rapid breathing, >25 breaths per min), auscultatory findings consistent with pneumonia, leucocytosis (white blood cell count >15×109 white blood cells/litre or >15% bands), serum procalcitonin above ≥0.5 mg/mL or hypoxaemia (O2 saturation <90% breathing room air or PaO2 <60 mm Hg), were considered a suspected case of pneumonia, and had a chest X-ray performed to further evaluate this diagnosis.

Only those with radiographically-confirmed CAP were considered as eligible for final inclusion in the study. The chest radiographs were interpreted by one board-certified chest radiologist (members of the research team, RB and CAdAN) at each site, who were unaware of the clinical data. Radiographic evidence of pneumonia was defined as the presence of a radiographic infiltrate in the lung parenchyma (eg, consolidation or other infiltrate, linear and patchy alveolar or interstitial densities), or pleural effusion.19

Patients were excluded if they had a clinical and radiographic picture that could be explained by an illness other than CAP, resided outside the study catchment area, had been enrolled before in this study (in the previous month) or presented criteria for healthcare-associated pneumonia (HCAP). We defined HCAP according to the American Thoracic Society and Infectious Diseases Society of America guidelines, including: any patient who was hospitalised in an acute care hospital for 2 or more days within 90 days of the infection; resided in a nursing home or long-term care facility; received recent intravenous antibiotic therapy, chemotherapy or wound care within the past 30 days of the current infection; or attended a hospital or haemodialysis clinic.20

Data collection

Patients and/or their caregivers were interviewed by trained staff, using a standardised questionnaire that included demographic data and information on lifestyle habits (smoking cigarettes, alcohol intake and substance abuse), and underlying medical conditions (asthma, chronic obstructive pulmonary disease, chronic heart disease, hypertension, HIV infection, diabetes mellitus, chronic kidney disease, history of stroke, chronic hepatitis and immunosuppression including cancer and immunosuppressive medication). Questions also included information on clinical signs and symptoms, antimicrobial use prior to hospitalisation and previous immunisations (self-reported vaccination against pneumococcus or against influenza vaccine during the last influenza season).

Specimen collection and laboratory testing

Blood samples, urine samples and nasopharyngeal swabs were obtained from the patients within 2 hours of attending the emergency department. In the case of patients with a productive cough, sputum was also obtained. Blood for culture was collected in BACTEC bottles, transported to a local certified laboratory HSR Lab (Hospital San Rafael Microbiology Laboratory, Salvador, Brazil). Urine samples for pneumococcal antigen detection were collected in a standard sterile specimen cup, refrigerated at 4°C for up to 4 hours after collection, aliquoted, stored at −70°C and shipped to Pfizer Vaccine Research and Development, (Pearl River, New York, USA,). S. pneumoniae was identified via BinaxNOW (Abbott) performed following the manufacturer’s recommendations.21 We also tested the urine samples with Luminex technology-based multiplex (UAD) diagnostic assays, UAD-1, to detect the S. pneumoniae serotypes 1, 3, 4, 5, 6A, 6B, 7F, 9V, 14, 18C, 19A, 19F and 23F (covered by PCV13), and UAD-2, to detect 11 additional serotypes, including the remaining serotypes covered by the 20-valent pneumococcal conjugate vaccine (PCV20) (8, 10A, 11A, 12F, 15B, 22F and 33F), licensed in the USA only, and the PPV23 (2, 9N, 17F and 20). Both assays were performed at Pfizer as described elsewhere.22 23

Nasopharyngeal specimens were collected using sterile swabs with flexible shafts, then they were promptly tested with a rapid diagnostic kit (QuickVue Influenza Test; Quidel, San Diego, California) using monoclonal antibodies specific for influenza A and B virus antigens. The test was performed at each participating site as instructed by the manufacturer.24 When available, sputum was collected into sterile containers. Gram stain, Ziehl–Neelsen stain and bacterial culture were performed at a local laboratory (HSR Lab). Only bacterial culture from sputum of high quality (≤10 epithelial cells/low power field (lpf) and ≥25 white blood cells/lpf) were included.25 Mycobacterium tuberculosis was considered a pathogen if detected in any acid-fast bacilli sputum specimen.

S. pneumoniae serotyping

Capsular serogroups/serotypes were deduced using multiplex-PCR as described elsewhere.26 All isolates identified as serogroup 6 in the multiplex-PCR were subjected to wciN6C-specific PCR, as previously described, for the identification of potential serotype 6C and 6D isolates.27 Isolates with negative or equivocal multiplex PCR results were subjected to Quellung reaction testing for capsular type definition.

Statistical analysis

Initially, a descriptive analysis of demographics and predisposing conditions for CAP was performed. Data were presented as frequencies and percentages for categorical variables and as median (IQR) for continuous variables. Incidence rates (expressed per 10 000 person-years) and 95% CIs were estimated with the Poisson exact method28 overall, and for each of the age categories. First, we adjusted the number of CAP cases, according to age group, for the proportion of eligible adults enrolled at both study sites (72%), and for the proportion of Salvador’s population depending exclusively on healthcare from the public sector SUS (70%).29 This adjusted number was then divided by the estimated population in the catchment areas of the study sites for the corresponding year and age group. This denominator was obtained by multiplying available census data on Salvador’s population30 by the proportion of all admissions estimated by the catchment area (market share) of the study emergency hospitals. Based on data from SIH (Hospital Information System) and CNES (National Register of Heath Institutions from the public database DATASUS,31 32 the average annual market share of the emergency hospitals during the study period was 17.9% (11.1% at UPA-Barris and 6.8% at UPA-Brotas). Alternatively, we also estimated the denominator for the incidence rates by using census data for the corresponding year and age group, to sum the population living in the surrounding boroughs in the health district of each study emergency hospital, and the rates remained mostly unchanged (data not shown).

Coverage potentially afforded by different vaccines was calculated as the percentage of serotypes included in pneumococcal vaccines among the isolates obtained from CAP cases during the study period. All the statistical analyses were performed using the Stata statistical software (V.12) (StataCorp).

Ethics statements

This study was conducted in accordance with applicable laws and regulations including, but not limited to, the International Conference on Harmonization Guideline for Good Clinical Practice and the ethical principles of the Declaration of Helsinki.

Results

Overall, 10 190 adults 50 years or older were screened for pneumonia at the two study sites. Among 314 patients with a clinical presentation suggestive of CAP, 154 met eligibility criteria, including radiological findings, for CAP diagnosis and 111 (72%) of them were enrolled (figure 1). Participants were significantly more likely to be 60 years of age or older (p=0.04) and more likely to be women (p=0.02) as compared with those who were eligible but not enrolled (data not shown).

Figure 1

Screening, eligibility and enrolment of patients with community-acquired pneumonia, Salvador, Brazil, 2018–2020.

The median age of patients with CAP was 64 years (IQR, 57–73), 51% had a multiracial background and 60% had middle school education or less (table 1). Self-rated overall health was fair or poor in 41%. At least one predisposing condition was present in 67% of participants with CAP, and two or more in 40%. Cough, fever, dyspnoea and pleuritic pain were the most common clinical findings. Nearly one-third of study participants had been immunised against influenza during the last influenza season, and only 3% of patients 60 years or older received PPV23 on at least one occasion. Sixty per cent had a clinical score (CRB-65) prediction for hospital referral or admission. Of 111 adults with CAP, 21 (19%) were managed as outpatients, 90 (81%) were hospitalised and none were admitted to the intensive care unit.

Table 1

Characteristics of middle aged and older adults with community-acquired pneumonia, Salvador, Brazil, 2018–2020

During the 2-year surveillance period, the annual incidence rate of CAP among adults 50 years or older requiring an emergency department visit was 20.1 cases (95% CI 17.6 to 22.7) per 10 000 adults (table 2). The incidence overall increased with increasing age, rising from 15.1 cases per 10 000 adults in participants 50–59 years old to more than three times higher among those 80 years or older, 54.4 (95% CI 36.8 to –76.6) per 10 000 adults. S. pneumoniae was the pathogen detected with the highest incidence, 7.6 cases (95% CI 6.1 to 9.2) per 10 000 adults. Ranging from 7.3 cases (95% CI 5.3 to 10.3) per 10 000 adults age 50 to 59 years to 13.5 cases (95% CI 6.3 to 29.8) per 10 000 adults 80 years or older.

Table 2

Estimated annual incidence rates of community-acquired pneumonia, Salvador, Brazil, 2018–2020‡*

Blood for culturing was obtained from all 111 adults with radiographic evidence of pneumonia, a specimen for urinary antigen detection from 106 (96%), a sputum specimen from 87 (78%) (of whom 74 (67%) had a high-quality specimen) and nasopharyngeal swabs from 85 (77%). All specimens were obtained before the administration of antibiotic agents. A pathogen was detected in 62 patients (56% of the CAP cases): one or more bacteria were detected in 51 patients (46%), influenza virus in 5 (4%), both bacterial and influenza virus in 3 (3%) and Mycobacteria in 3 (3%) (figure 2). S. pneumoniae was detected in 38% (42/111) participants as determined by BinaxNOW, UAD, or culture. S. pneumoniae was detected by culture alone in 11% (12/111), by UAD alone in 10% (11/111) patients, and by BinaxNOW alone in 5% (6/111) cases. Another 12% (13/111) cases were detected by any combination of these three diagnostic methods (figure 3).

Figure 2

Pathogen detection among middle aged and older adults with community-acquired pneumonia, Salvador, Brazil, 2018–2020.

Figure 3

Diagnostic method for Streptococcus. pneumoniae identification among all study participants with radiographically-confirmed community-acquired pneumonia (n=111). A total of 42 (38%) had S. pneumoniae detected by any method. UAD, proprietary serotype-specific urinary antigen detection assay. The UAD only detects 24 serotypes contained in licenced pneumococcal vaccines.

A serotype of S. pneumoniae was identified via culture or UAD in 36 of 42 (86%) cases of pneumococcal CAP, while six cases diagnosed by BinaxNOW alone could not be typed. The distribution of the 17 different serotypes detected is shown in figure 4. The most commonly identified serotypes were 3, 9N and 4. They comprised about one-third of CAP caused by pneumococcus, and were found in 15 of 111 (13.5%) patients with all-cause CAP. The percentage of pneumococcal CAP caused by vaccine serotypes increased with the number of serotypes included in the formulation as follows: 23.8% (PCV10), 47.6% (PCV13), 59.5% (PCV20) and 71.4% (PPV23). Among patients with all-cause CAP, the potential coverage afforded by different pneumococcal vaccines was 9.0% (PCV10, not licenced for adults), 18.0% (PCV13), 22.5% (PCV20, licenced in the USA only) and 27.0% (PPV23), as shown in table 3.

Table 3

Coverage of pneumococcal vaccines serotypes among middle aged and older adults with community-acquired pneumonia, Salvador, Brazil, 2018–2020

Figure 4

Serotype distribution of Streptococcus pneumoniae isolates (n=42) among middle aged and older adults with community-acquired pneumonia, Salvador, Brazil, 2018–2020.

Discussion

In this prospective study, we have assessed the population-based incidence and the aetiology of CAP among adults 50 years or older requiring an emergency department visit in Brazil during a consecutive 24-month study period. The incidence of radiologically confirmed CAP varied from 23.6 to 16.7 per 10 000 person-years in the first and second year of study, respectively; though the rates of influenza reported in these 2 years were similar.33 Age group-specific incidence rates increased with advancing age to 54.4 per 10 000 person-years in the 80 years or older age group. These estimates are similar to the annual incidences reported in the USA (20.6 and 29.2 per 10 000 person-years) by Jain et al,8 and are lower than a previous report in three cities in South America that found CAP incidences in adults aged ≥18 years varying from 17.6 to 70.3 per 10 000 person-years; in particular, for adults older than 65 years, incidence ranged from 109.0 to 294.9 per 10 000 person-years.6 The rates in our study are higher than those in a review of studies from several European countries where the incidence of CAP in adults ranged between 10.7 to 12.0 per 10 000 person-years and from 15.4 to 17.0 per 10 000 population. In the age group older than 65 years, CAP incidence in Spain ranged from 127 to 153 per 10 000 person-years.34 With respect to hospitalisation, in a retrospective, web-based database study in Brazil, the incidence per 10 000 of hospitalisation due to all-cause pneumonia decreased from 45.1 in 2003 to 38.8 in 2007.5 In another study, the incidence of hospitalised and outpatient pneumonia in Brazil was 61.1 and 70.6 per 10 000 inhabitants/year, respectively.35

The wide variation in the incidence rates of CAP in previous reports may be explained by differences in study design, definition of CAP, enrolment criteria, study procedures, incidence estimations and surveillance methods. In addition, differences in demographic characteristics and/or in the provision of and access to healthcare make it difficult to compare results across different studies. Variation in CAP incidence depending on age, lifestyle habits such as smoking and alcohol consumption and chronic illnesses may also reflect true differences in these determinants between populations. Of note, hypertension was the most frequent underlying condition reported in our survey, that hypertension has not been identified previously as a risk factor for CAP. Furthermore, some retrospective studies are limited to the identification of CAP cases through registries with general codes that often include unconfirmed cases, nosocomial pneumonias, readmissions and hospitalisations due to other causes.36 37 The CAP incidence estimates reported here result from thorough ascertainment of cases during the active, prospective surveillance. Moreover, due to the exclusion of recently hospitalised patients and the increased specificity of radiographic confirmation in our case definition, it is unlikely that our rates are overestimated.

With respect to vaccination, there was a 31% coverage for influenza and a 3% coverage for pneumococcal vaccines (3%) in our study population, while universal pneumococcal vaccination in infants may reduce the incidence of pneumococcal diseases in adults through herd protection.38 The impact of herd protection offered by vaccination in children varies in different populations depending on introduction of pneumococcal vaccination in national programmes and its coverage.

A microbial aetiology could be identified for 56% of the patients. Overall, our pathogen-detection yield is within the range (38%–70%) of the yield in other aetiological studies of pneumonia in adults.8 39–41 In a study combining a new diagnostic PCR platform with conventional methods in Sweden,39 respiratory viruses were identified in 29% of patients with CAP, and identified in 34% of CAP in hospitalised adults in a 3-year prospective study in Norway.40 The prompt collection of specimens for bacteria cultures might have improved the detection rates for these pathogens in our study, whereas the limited investigation of viruses likely led to missing diagnosis for these agents. Like other studies using broad diagnostic methods,8 39–41 several cases of CAP remained with no causative organism identified. Possible reasons for that include previous antibiotic use, failure to obtain lower respiratory tract specimens, insensitive diagnostic tests for known pathogens, a lack of testing for virus other than influenza and unidentified pathogens.18 42

S. pneumoniae was the most detected pathogen (38%) in our study. Pneumococcus is a common cause of CAP in adults10 and has been reported as a leading cause of CAP, with 9%–48% prevalence in other studies.43 44 Serotype 3 was the predominant pneumococcus identified in our sample. This serotype remains a major cause of invasive pneumococcal disease in England and Wales,45 despite its inclusion in PCV13. Vaccine effectiveness has been reported as non-significant for this serotype, leading to it being recorded as a major vaccine evader.46

The majority (52%) of pneumococcal infections in our study were detected by urinary antigen tests for pneumococcus alone (UAD and/or BinaxNOW). These tests are more sensitive than blood culture and improve the detection of non-bacteraemic pneumococcal pathogens.22 25 47 Influenza virus was the second most common (7%) pathogen detected in our study. Noteworthy, just 31% of participants had received influenza vaccine during the past influenza season. This might have contributed to the observed frequency of this virus and emphasises the need for improvements in influenza-vaccine uptake in our population.

About a quarter of cases of all-cause CAP were attributable to serotypes included in currently licenced pneumococcal vaccines; thus, these cases could have been potentially prevented by vaccination. Of note, the serotype-specific UAD assays used in this study were designed to only detect the 24 serotypes contained in licenced pneumococcal vaccines, which may have led to an underestimation of the proportion of CAP due to non-vaccine pneumococcal serotypes. Given the higher sensitivity of these assays for detecting pneumococcal serotypes compared with traditional culture methods,22 23 48 our study likely overestimates the proportion of pneumococcal disease due to vaccine serotypes.

Reports on the prevalence of pneumococcal serotypes often rely on studies using culture-based diagnostic methods that can only identify a reduced fraction of CAP with bacteraemia; thus, being limited to invasive pneumococcal disease. Along with conventional culture-based methods, this study is the first to use the proprietary serotype-specific urinary antigen detection assays (UAD-1 and UAD-2) to assess the distribution of vaccine pneumococcal serotypes associated with adult CAP in Brazil. These assays provided increased sensitivity over methods in previous studies, while ensuring a more thorough description of the prevalence of pneumococcal serotypes and better understanding of pneumococcal CAP epidemiology.

The study has some limitations. One is a potential underidentification of CAP events. It is possible that some patients with mild symptoms were missed because they were treated in outpatient clinics and did not seek an emergency department for evaluation. In addition, some eligible patients declined to participate or were not able to consent. However, the incidence calculations were adjusted for the enrolment differences according to age. Another limitation concerns the design of the study as viral diagnosis only included detection of influenza. Use of extensive viral testing could have afforded a better understanding of CAP epidemiology. Nevertheless, all patients had at least one specimen type available for bacterial detection, obtained before the administration of antibiotic agents. Lastly, one more limitation of this study is that, although our data from two large public hospital includes a diverse population, overall the study population includes only persons depending exclusively on healthcare from the public sector SUS and living in a single geographical area population. Thus, it may not be possible to extrapolate our findings to the entire Brazilian adult population, since the epidemiology of respiratory infections varies according to geographical region, timing and other determinants.

The main strength of this study lies in its methodological design. It was an active, prospective, population-based study conducted over a period of two consecutive years. We used outcome measures and definitions based on specified criteria, and the study procedures were standardised and completed in almost all subjects. In addition, all cases of CAP were radiographically confirmed and validated by clinical information. We also employed non-culture-based tests (UAD) to improve the detection of S. pneumoniae in non-bacteraemic cases of CAP.

In conclusion, this study assessed the burden of CAP and provided reliable estimates for the incidence rates of CAP requiring an emergency department visit among adults in Brazil. Moreover, the serotype distribution of S. pneumoniae causing pneumonia allowed an estimate of the potential coverage afforded by different licenced pneumococcal vaccines, a crucial information for the overall impact of pneumococcal vaccination programmes, as well as appropriate decision-making processes for informing current immunisation policy. Continual surveillance is essential to monitor trends in incidence and serotype distribution, and to understand potential impact and value of high-valency pneumococcal conjugate vaccines. Pneumococcus and influenza were frequently detected, which probably reflect the lack of direct benefit of specific vaccination against these pathogens and suggest that improving the coverage and effectiveness of recommended influenza and pneumococcal vaccines could reduce the burden of pneumonia among adults.

Data availability statement

Data are available upon reasonable request.

Ethics statements

Patient consent for publication

Ethics approval

The study protocol was approved by the Ethics Committee of the Santo Antônio Hospital (Approval #: CAAE56884916.9.0000.0047). Participants gave informed consent to participate in the study before taking part.

Acknowledgments

The authors wish to thank all subjects who took part in the study. We are also in debt to the staff at the participating facilities during the sample collection for their valuable collaboration.

References

Footnotes

  • FGD and MGB contributed equally.

  • Contributors FGD, MGB, SdSM, JNR, JRS, RSdA, RA-P, RB, CAdAN and EDM developed the study concept and design. SdSM coordinated the study and gathered participants. FGD and EDM carried out the data analysis. FGD and MGB drafted the manuscript. All authors contributed to the interpretation of the results, provided comments and revisions. All authors read and approved the final manuscript. EDM is the guarantors of this work and takes responsibility for the integrity of the data and the accuracy of the data analysis.

  • Funding This work was supported by an unrestricted grant from Pfizer, São Paulo, Brazil (Grant WI219729). This study was conducted as a collaboration between Associação Obras Sociais Irmã Dulce and Pfizer.

  • Competing interests JRS, RSdA, KEA and RA-P are employed by Pfizer and have ownership interests in Pfizer. EDM Junior has served on advisory board member for Pfizer and has received grant support through his institution from Pfizer Inc. All other authors declare no conflict of interest.

  • Patient and public involvement Patients and/or the public were not involved in the design, or conduct, or reporting, or dissemination plans of this research.

  • Provenance and peer review Not commissioned; externally peer reviewed.