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Burden of respiratory syncytial virus hospitalisation among infants born at 32–35 weeks' gestational age in the Northern Hemisphere: pooled analysis of seven studies

Published online by Cambridge University Press:  17 August 2020

M. Lanari
Affiliation:
Pediatric Emergency Unit, Department of Medical and Surgical Sciences, S. Orsola University Hospital, Bologna, Italy
E.J. Anderson
Affiliation:
Departments of Pediatrics and Medicine, Emory University School of Medicine, Atlanta, GA, USA
M. Sheridan-Pereira
Affiliation:
Department of Paediatrics, Trinity College and Coombe Women and Infants University Hospital, Dublin, Ireland
X. Carbonell-Estrany*
Affiliation:
Neonatology Service, Hospital Clinic, Institut d'Investigacions Biomediques August Pi Suñer (IDIBAPS), Barcelona, Spain
B. Paes
Affiliation:
Department of Pediatrics (Neonatal Division), McMaster University, Hamilton, Ontario, Canada
B.S. Rodgers-Gray
Affiliation:
Strategen Limited, Winchester, UK
J. R. Fullarton
Affiliation:
Strategen Limited, Winchester, UK
E. Grubb
Affiliation:
Health Economics and Outcomes Research, AbbVie Inc, North Chicago, Illinois, USA
M. Blanken
Affiliation:
Division of Pediatric Immunology and Infectious Diseases, University Medical Center Utrecht, Utrecht, The Netherlands
*
Author for correspondence: X. Carbonell-Estrany, E-mail: carbonell@comb.cat
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Abstract

To provide comprehensive information on the epidemiology and burden of respiratory syncytial virus hospitalisation (RSVH) in preterm infants, a pooled analysis was undertaken of seven multicentre, prospective, observational studies from across the Northern Hemisphere (2000–2014). Data from all 320–356 weeks' gestational age (wGA) infants without comorbidity were analysed. RSVH occurred in 534/14 504 (3.7%) infants; equating to a rate of 5.65 per 100 patient-seasons, with the rate in individual wGA groups dependent upon exposure time (P = 0.032). Most RSVHs (60.1%) occurred in December–January. Median age at RSVH was 88 days (interquartile range (IQR): 54–159). Respiratory support was required by 82.0% of infants: oxygen in 70.4% (median 4 (IQR: 2–6) days); non-invasive ventilation in 19.3% (median 3 (IQR: 2–5) days); and mechanical ventilation in 10.2% (median 5 (IQR: 3–7) days). Intensive care unit admission was required by 17.9% of infants (median 6 days (IQR: 2–8) days). Median overall hospital length of stay (LOS) was 5 (IQR: 3–8) days. Hospital resource use was similar across wGA groups except for overall LOS, which was shortest in those born 35 wGA (median 3 vs. 4–6 days for 32–34 wGA; P < 0.001). Strategies to reduce the burden of RSVH in otherwise healthy 32–35 wGA infants are indicated.

Type
Original Paper
Creative Commons
Creative Common License - CCCreative Common License - BY
This is an Open Access article, distributed under the terms of the Creative Commons Attribution licence (http://creativecommons.org/licenses/by/4.0/), which permits unrestricted re-use, distribution, and reproduction in any medium, provided the original work is properly cited.
Copyright
Copyright © The Author(s), 2020. Published by Cambridge University Press

Introduction

Respiratory syncytial virus (RSV) remains a leading cause of lower respiratory tract infection (LRTI) in early childhood [Reference Bont1], causing over 375 000 hospitalisations (respiratory syncytial virus hospitalisation (RSVHs)) per year in children <5 years in high-income countries [Reference Shi2]. RSVHs are concentrated during seasonal outbreaks – the winter months in temperate countries – and place a major demand on neonatal and paediatric services at this time of year [Reference Thwaites3]. Certain children, such as those with co-morbidities, including congenital heart disease and chronic lung disease, immunodeficiency and those born prematurely, are known to be particularly vulnerable to severe RSV LRTI [Reference Checchia4Reference Figueras-Aloy6].

An important group that has generated much debate comprises those children born 32–35 weeks' gestational age (wGA), in terms of their level of risk for RSVH compared to those born at lower and higher wGA and the cost-effective deployment of prophylaxis with palivizumab [Reference Paes, Rodgers-Gray, Carbonell-Estrany and Resch7]. This is reflected in international guidelines, with some, such as from the American Academy of Pediatrics [8, Reference Munoz9], not recommending RSV prophylaxis in 32–35 wGA infants, while others, such as from Spain and Italy [Reference Figueras Aloy10, Reference Bollani11], recommending the use of risk factors to guide prophylaxis in 32–35 wGA infants at highest risk. Palivizumab currently represents the only licensed and effective prophylaxis for preventing RSVH in high-risk infants, including those born 32–35 wGA, although several promising monoclonal antibody candidates could become available in the next few years [Reference Simões12]. A comprehensive understanding of the risk and burden of RSVH in otherwise healthy 32–35 wGA infants is important to help guide preventive interventions.

A number of prospective studies have assessed the burden of RSVH in children born 32–35 wGA within Northern Hemisphere countries [Reference Figueras-Aloy13Reference Straňák19]. To provide a greater understanding of the burden of RSVH across the Northern Hemisphere, we previously analysed pooled data from seven studies that focused on 33–35 wGA infants born and hospitalised during the RSV season [Reference Anderson20]. In total, 267 out of 7820 (3.4%) 33–35 wGA infants were hospitalised for RSV during the RSV season, with an overall rate of 4.5 per 100 patient-seasons. The median hospital length of stay (LOS) was 6 days, and 22% required intensive care unit (ICU) admission for a median of 8 days. Supplemental oxygen support was required by 70.4% of infants for a median of 5 days and 12.7% required mechanical ventilation for a median of 5 days [Reference Anderson20].

Herein we analysed those born at 32 wGA, stratified results across individual wGA, and assessed those born and hospitalised outside of the RSV season.

Methods

Included studies

The selection of studies comprising the pooled dataset has been described previously [Reference Anderson20]. Briefly, studies of RSVH in 32–35 wGA infants (defined as 32 weeks and 0 days (320) to 35 weeks and 6 days (356)) were identified via a systematic search of PubMed and EMBASE from January 1998 to January 2015. Study selection criteria included a multicentre, observational, prospective design; inclusion of >1000 preterm infants; and laboratory-confirmed RSV infection in all subjects (direct immunofluorescence assay, rapid antigen/enzyme membrane testing, rapid shell viral detection or polymerase chain reaction (PCR)-based assays), who were hospitalised with an LRTI. Studies where >15% of infants received palivizumab prophylaxis were excluded (to standardise and to avoid potential confounding) and only one study (most recent) from an individual country was included (to limit data to one representative study from each country). The overall aim was to include large, high-quality, cross-sectional studies that, when combined, provide an overview of the burden of RSV generalisable across the Northern Hemisphere.

The original review comprised seven studies (spanning 2000–2014) [Reference Anderson20], and no additional reports were identified when the searches were updated to 31 January 2020. The seven studies were as follows: Risk Factors Linked to Respiratory Syncytial Virus Infection Requiring Hospitalization in Premature Infants Study (FLIP-2, Spain) [Reference Figueras-Aloy13]; RISK Study (the Netherlands) [Reference Blanken14]; Pediatric Investigators Collaborative Network on Infections in Canada (PICNIC, Canada) [Reference Law15]; RSV Preterm Risk Estimation Measure for RSV Hospitalization in Ireland (RSV-PREMI, Ireland) [Reference Sheridan-Pereira16]; Italian National Birth Cohort (IBC, Italy) [Reference Lanari17]; RSV Respiratory Events among Preterm Infants Outcomes and Risk Tracking (REPORT, USA) [Reference Ambrose18]; and Predictors Associated with RSV HOspitalization in Nonprophylaxed, Premature Infants (PONI, multinational) [Reference Straňák19].

Cohort selection

All 320–356 wGA infants (≤1 year) were included in this analysis except: those with a comorbidity associated with an increased risk of RSVH (e.g. Down syndrome, immunodeficiency, congenital heart disease, bronchopulmonary dysplasia); those who had received palivizumab prophylaxis; and those with an RSV-negative respiratory-related hospitalisation. Gestational age was determined within each study based on standard criteria, namely ultrasonographic dating and/or the time between the first day of the last menstrual period and delivery date.

Pooled analysis

The individual datasets from the seven studies were previously shown to be homogeneous when analysed in 33–35 wGA infants born and hospitalised during the RSV season [Reference Anderson20]. Predicated on this, for the current analysis, data were amalgamated and analyses performed on the combined dataset without weighting. All seven studies contained data on infants born 33–35 wGA, while four (FLIP-2, PREMI, REPORT and RISK) also included 32 wGA infants (Table 1). Age at first RSVH and distribution of RSVHs by month were calculated using data from studies that had year-round surveillance (FLIP-2, IBC, PREMI and RISK), while results stratified by wGA used data only from those studies that included 32 wGA infants (FLIP-2, PREMI, REPORT and RISK).

Table 1. Overview of included studies

RSV, respiratory syncytial virus; wGA, weeks' gestational age (superscript digit indicates days).

a PONI countries: Austria, Bahrain, Czech Republic, Egypt, Estonia, France, Jordan, Korea, Latvia, Lebanon, Lithuania, Mexico, Norway, Oman, Portugal, Russia, Saudi Arabia, Slovakia, Slovenia, Sweden.

Outcomes

RSVH frequency was expressed as both an incidence rate and as a rate per 100 patient-seasons, with the latter adjusted for length of exposure during the RSV season for the full cohort (NB in our previous analysis restricted to 33–35 wGA infants born and hospitalised within the RSV season +1 month, the exposure rate used was for RSVH cases only [Reference Anderson20]). Season start and end dates were taken from each study and confirmed with the respective study leads, and ranged between 1 October and 30 April (Table 1). RSVHs were further stratified by month during the RSV season and by wGA. RSVH in relation to chronological age was also assessed split by those born during and outside the RSV season.

The following outcomes related to RSVHs were assessed: requirement for and duration of oxygen support; requirement for and duration of other non-invasive respiratory support/ventilation (defined as the use of high-flow nasal cannula, continuous positive airway pressure and/or nasal intermittent positive pressure ventilation/non-invasive positive pressure ventilation); requirement for and duration of mechanical ventilation (defined as any intervention that included intubation or extracorporeal membrane oxygenation); admission to and LOS in ICU; and overall hospital LOS.

Statistical analysis

LOS and duration of respiratory support required were expressed as a median with interquartile range (IQR). Length of follow-up was presented as a mean plus standard deviation (SD). RSVH incidence rates were compared using the Kruskal–Wallis test and Spearman (non-parametric) correlation. Differences in hospital resource use by wGA were assessed using the Kruskal–Wallis test. Analyses of partial seasonal exposure in relation to RSVH across gestational age groups were carried out using Cox regression. Analyses were performed using SPSS for Windows version 15.0 (SPSS Inc, Chicago, IL, USA), Microsoft Access SQL (Microsoft, Redmond, WA, USA) and/or Microsoft Access/Excel VBScript (Microsoft). A P-value <0.05 was considered statistically significant.

Results

Pooled dataset

In total, the pooled analysis included 14 504 infants born between 320 and 356 wGA, for which year-round data were available for 9020 (Fig. 1). For the analyses split by wGA (n = 9686) there were: 1046/9686 (10.8%) infants born at 32 wGA, 2235/9686 (23.1%) at 33 wGA, 3646/9686 (37.6%) at 34 wGA and 2759/9686 (28.5%) at 35 wGA.

wGA, weeks' gestational age; *9 cases which were not hospital confirmed, 11 where there was no record of wGA.

Fig. 1. Derivation of pooled dataset.

Epidemiology of RSVH

Overall

Of the 14 504 infants, 534 had a confirmed RSVH, representing an incidence of 3.7%. The corresponding rate per 100 patient-seasons was 5.65. December and January accounted for over half of RSVHs (60.1%), with 94.1% of RSVHs occurring between November and March (Fig. 2); across a mean follow-up of 204.1 (SD: 104.9) days. In total, 2.4% (9/371) of RSVHs occurred outside the RSV season. RSVH incidence rates were similar for those born within and outside the RSV season (4.3% vs. 3.9%, respectively; χ 2: P = 0.25). Overall, 42.3% of RSVHs (157/371) occurred in infants born outside the RSV season.

RSVH, respiratory syncytial virus hospitalisation. *Data from FLIP-2, IBC, PREMI and RISK (studies with year-round data capture). Total RSVHs: 371.

Fig. 2. Distribution of RSVH incidence by month*

Median age at RSVH was 88 (IQR: 54–159) days, with approximately half of RSVHs (52.6%; 195/371) occurring in infants <3 months old and four-fifths occurring in infants ≤6 months old (81.7%; 303/371). For those born within and outside the RSV season, the median age at RSVH was 62 (IQR: 40–96) days and 143 (IQR: 94–188) days, respectively.

Analysis by wGA

RSVH incidence tended to increase with decreasing wGA at birth, although this did not reach statistical significance: 4.0% for those born 35 wGA; 4.0% for 34 wGA; 4.7% for 33 wGA; and 5.0% for 32 wGA (χ 2: P = 0.09; Spearman: P = 0.10). However, when converted to a rate per 100 patient-seasons, the difference between wGA groups was significant (Spearman: P = 0.03): 35 wGA 5.66; 34 wGA 6.14; 33 wGA 7.29; and 32 wGA 7.84. The length of seasonal exposure to RSV also increased with increasing wGA (Spearman: P = 0.003). Cox regression analysis showed an upward trend in mean seasonal exposure rates amongst RSVH cases between 32 wGA (0.638) and 35 wGA (0.707) and the Wald statistic for seasonal exposure as a predictor of change in hazard for RSVH was highly significant (P < 0.001) in every group. The proportion of RSVHs outside the RSV season did not differ significantly with wGA, albeit there was a rising rate with increasing wGA (32 wGA: 0.0%; 33 wGA: 2.0%; 34 wGA: 2.3%; 35 wGA: 2.7%; Spearman: P = 0.36). Median age at RSVH did not significantly differ across wGA groups (Spearman: P = 0.21), although infants born at 32 wGA (118 (IQR: 64–195) days) seemed to have an extended period of risk compared to those born at ³33 wGA (33 wGA: 82 (IQR: 55–153) days; 34 wGA: 91 (IQR: 51–154) days; 35 wGA: 89 (IQR: 47–159)).

Healthcare resource use during RSVH

Overall

Four out of five infants (82.0%; 260/317) required some form of oxygen therapy or respiratory support during their RSVH; 70.4% required supplemental oxygen, 19.3% non-invasive ventilation and 10.2% mechanical ventilation (Table 2). Supplemental oxygen was used for a median of 4 (IQR: 2–6) days, non-invasive ventilation for 3 (IQR: 2–5) days and mechanical ventilation for 5 (IQR: 3–7) days. Of the cases, 17.9% were admitted to the ICU for a median of 6 (IQR: 2–8) days. Overall hospital LOS was for a median of 5 (IQR: 3–8) days.

Table 2. Healthcare resource use during RSVH

ICU, intensive care unit; IQR, interquartile range; N/A, not applicable.

N represents all those with available data for specific variables in the pooled dataset.

a Pooled data from: FLIP-2, IBC, PREMI, RISK, PONI, REPORT and PICNIC.

b Pooled data from: FLIP-2, PREMI, REPORT and RISK.

Analysis by wGA

The percentages of infants requiring any form of respiratory support were highest in those born most premature, although results were not significantly different across wGA groups: 59.6% (31/52) for those born 32 wGA; 50.5% (53/105) for 33 wGA; 44.1% (64/145) for 34 wGA; and 43.6% (48/110) for 35 wGA (Kruskal–Wallis: P = 1.000; Spearman: P = 0.06). None of the other hospital resource variables differed significantly between 32, 33, 34 and 35 wGA infants except the median duration of overall hospital LOS, which was lower (P < 0.001) for those born 35 wGA (3 (IQR: 2–6) days) after a progressive increase in stay from 32 to 34 wGA (32: 4 (3–7) days; 33: 5 (3–8) days; 34: 6 (4–9) days).

Discussion

This pooled analysis of 14 504 infants provides a comprehensive evaluation of the epidemiology and burden of RSVH in 32–35 wGA infants in the Northern Hemisphere. The overall incidence of RSVH was 3.7% and the overall rate per 100 patient-seasons was 5.65, with over half (60.1%) of all RSVHs occurring in December and January. While the asserted start and end dates of the RSV season varied by country (and sometimes within the country) and year-to-year, the main at-risk period spanned from November through March (94.1% of all RSVHs).

While RSVH incidence did not significantly differ with wGA (P = 0.10), the rate per 100 patient-seasons did significantly increase with decreasing wGA (35 wGA 5.66; 34 wGA 6.14; 33 wGA 7.29; 32 wGA 7.84; P = 0.032). Other studies, such as those from Denmark [Reference Haerskjold21] and the USA [Reference Anderson22], have reported increasing RSVH incidence rates with decreasing wGA. A Dutch community-based cohort study reported that overall RSVH rates of 32–36 wGA infants (n = 964, 3.9%) were greater than full-term infants (38–42 wGA; n = 572, 1.2%; relative risk (RR) 3.2, 95% CI 1.4–7.1), but equal to <32 wGA infants (n = 524; 3.9% vs. 3.2%, RR 1.2, 95% CI 0.7–2.1) [Reference Gijtenbeek23]. Our study suggests that a key factor when comparing RSVH rates across wGA groups is the length of exposure to RSV, with more premature infants in our analysis requiring a shorter exposure time to be admitted for LRTI (Spearman: P = 0.003; Cox: P < 0.001).

The median age at RSVH was approximately 3 months (88 days), with half (53%) of all RSVHs occurring in those <3 months of age and four-fifths in those ≤6 months of age (82%). The median age at RSVH did not differ significantly across wGA (P = 0.21), although infants born 32 wGA appeared to have a longer at-risk period (median 118 days) than those born 33–35 wGA (82–91 days). Similar results were reported in the US SENTINEL 1 study, where the median age at RSVH was 3 months for 29–32 wGA infants and 2 months for 33–35 wGA infants [Reference Anderson22]. Among 29–32 wGA infants, 55% of RSVHs occurred in those <4 months of age, and among 33–35 wGA infants, 55% of RSVHs occurred in those <3 months of age [Reference Anderson24]. In total, 78% of RSVHs in 29–35 wGA infants were in those <6 months old [Reference Anderson25]. Another US study, including preterm and term infants, reported that 64% of RSVHs occurred in infants ≤5 months old [Reference Hall26]. The RSVH incidence rates in our study were similar whether the infants were born within or outside the RSV season (4.3% vs. 3.9%; P = 0.25), possibly reflecting younger chronological age in the former balanced against the increased duration of exposure in the latter.

RSVHs were associated with considerable resource use, with 82% of infants requiring some form of respiratory support, 10% mechanical ventilation for a median of 5 days and 18% ICU admission for a median of 6 days. Studies from the USA, including SENTINEL 1, have reported higher ICU admission rates of 40–50% in similar wGA infants [Reference Anderson25, Reference Horn and Smout27], albeit comparable ICU LOS (5–7 days) [Reference Anderson25]. Overall hospital LOS was also comparable in our study to SENTINEL 1 (median 5 vs. 5–6 days [Reference Anderson25], respectively). It has been reported that 33–35 wGA infants had significantly higher resource use during RSVH than those born ≤32 or ⩾36 wGA [Reference Horn and Smout27], though this has not been substantiated in other studies. Interrupted lung development during the critical period before 36 wGA and immunologic immaturity are potential contributors to an increased RSVH risk [Reference Langston28, Reference Friedrich29]. In our study, hospital resource use was broadly similar across each wGA group, although 35 wGA infants, on average, spent less overall time in hospital than their younger wGA counterparts (median 3 vs. 4–6 days, respectively; P < 0.001). The costs associated with an RSVH episode in preterm infants have been estimated at a median $14 000–77 000 in the USA [Reference Anderson22, Reference Anderson25] and €2000–4000 in Europe [Reference Blanken30]. After RSVH discharge, 32–35 wGA infants continue to have substantial medical expenses [Reference Palmer31, Reference Sampalis32].

The main limitations of our pooled analysis were related to some salient differences in methodology/design of the included studies. Most notably, only four of seven studies included 32 wGA infants, although data were available on >1000 such infants. Other differences included the fact that the PICNIC study enrolled only infants born and hospitalised during the RSV season (+1 month) and variable lengths of follow-up (Table 1). Heterogeneity between datasets was previously reported for age at admission (non-parametric Levene test: P = 0.001) and duration of hospitalisation (non-parametric Levene test: P < 0.001) [Reference Anderson20]. The studies spanned 2000–2014 and RSV diagnostic tests have evolved during this period, with the earlier studies predominantly using direct immunofluorescence assay, rapid antigen/enzyme membrane testing and rapid shell viral detection, whilst the later studies used more sensitive PCR-based assays. Differences in admission criteria and medical practice between countries as well as cultural factors, such as frequency and earlier enrolment in day care, a recognised risk factor for RSVH, might also have influenced RSV admission rates across studies. For these reasons, the pooled analysis was undertaken without weighting and the analyses by wGA and age restricted to those studies that included 32 wGA infants and year-round surveillance, respectively. Despite some differences, the methodologies of the seven studies were broadly similar overall in terms of being multicentre, observational, prospective studies involving 32–35 wGA infants. It is also a strength that for five of the seven studies (FLIP-2, RISK, PICNIC, REPORT and PONI), representing 86% (12 449/14 504) of the total study population, RSV testing was part of the protocol [Reference Figueras-Aloy13, Reference Blanken14, Reference Law15, Reference Ambrose18, Reference Straňák19]. A high proportion (80%; 93/116) of LRTI cases were also RSV tested in PREMI (70% (65/93) positive) [Reference Sheridan-Pereira16]. In the Italian Birth Cohort [Reference Lanari17], a quarter (26%; 31/120) of cases were tested (84% (26/31) positive). Taken together, it can be seen that the pooled analysis provides an accurate representation of the true burden of RSVHs in otherwise healthy 32–35 wGA infants in the Northern Hemisphere.

Conclusion

Our study provides comprehensive data on the epidemiology and burden of RSVH in 32–35 wGA infants in the Northern Hemisphere that can help inform healthcare policy on the deployment of preventive strategies, such as palivizumab. The use of a country-specific or customisable risk factor scoring tool to identify the highest risk infants [Reference Blanken33] should be implemented, as recommended by recent expert consensus [Reference Sánchez Luna34]. Such strategies, together with the advent of RSV vaccine(s) and the potential for newer extended half-life monoclonal antibodies, could help to alleviate the burden of RSV LRTI in these at-risk infants.

Acknowledgements

The authors would like to acknowledge Dr Gerard Notario, Dr Pamela Vo and Fiona Campbell for their contribution to the first pooled analysis using these data. The authors would also like to thank Dr Matthew Freddi (Strategen Ltd) for editorial services, funded by AbbVie. Dr John Fullarton had full access to all of the data in the study and takes responsibility for the integrity of the data and the accuracy of the data analysis.

Financial support

Financial support for this study was provided by AbbVie. AbbVie participated in analysis and interpretation of data, drafting, reviewing and approving the publication.

Conflict of interest

EJA, ML, XC-E, MB, MS-P, BP have received research funding and/or compensation as advisor/lecturer from AbbVie. EJA has received research funding from MedImmune, Regeneron, Pfizer, Merck, Novavax, GSK, Sanofi Pasteur, PaxVax and Micron. EJA has received compensation from Pfizer for consulting. BRG and JF, working for Strategen, have previously received payment from AbbVie for work on various projects. EG is an employee of AbbVie and owns stock.

Data availability statement

Requests for access to the data that support this study should be made to the corresponding authors, XCE.

References

Bont, L et al. (2016) Defining the epidemiology and burden of severe respiratory syncytial virus infection among infants and children in western countries. Infectious Diseases and Therapy 5, 271298.CrossRefGoogle ScholarPubMed
Shi, T et al. (2017) Global, regional, and national disease burden estimates of acute lower respiratory infections due to respiratory syncytial virus in young children in 2015: a systematic review and modelling study. Lancet (London, England) 390, 946958.CrossRefGoogle ScholarPubMed
Thwaites, R et al. (2020) Clinical burden of severe respiratory syncytial virus infection during the first 2 years of life in children born between 2000 and 2011 in Scotland. European Journal of Pediatrics 179, 791799.CrossRefGoogle ScholarPubMed
Checchia, PA et al. (2017) Defining the risk and associated morbidity and mortality of severe respiratory syncytial virus infection among infants with congenital heart disease. Infectious Diseases and Therapy 6, 3756.CrossRefGoogle ScholarPubMed
Paes, B et al. (2016) Defining the risk and associated morbidity and mortality of severe respiratory syncytial virus infection among infants with chronic lung disease. Infectious Diseases and Therapy 5, 453471.CrossRefGoogle ScholarPubMed
Figueras-Aloy, J et al. (2016) Defining the risk and associated morbidity and mortality of severe respiratory syncytial virus infection among preterm infants without chronic lung disease or congenital heart disease. Infectious Diseases and Therapy 5, 417452.CrossRefGoogle ScholarPubMed
Paes, B, Rodgers-Gray, B and Carbonell-Estrany, X (2019) Resolving the debate on RSV prophylaxis in late preterm infants. In Resch, B (ed.), The Burden of Respiratory Syncytial Virus Infection in the Young. London, UK: IntechOpen, pp. 2944.Google Scholar
American Academy of Pediatrics Committee on Infectious Diseases; American Academy of Pediatrics Bronchiolitis Guidelines Committee (2014) Updated guidance for palivizumab prophylaxis among infants and young children at increased risk of hospitalization for respiratory syncytial virus infection. Pediatrics 134, 415420.CrossRefGoogle Scholar
Munoz, FM et al. (2017) RSV Recommendations unchanged after review of new data. AAP News 38, 14.Google Scholar
Figueras Aloy, J et al. (2015) Actualización de las recomendaciones de la Sociedad Española de Neonatología para la utilización del palivizumab como profilaxis de las infecciones graves por el virus respiratorio sincitial. Anales de Pediatría 82, e1e2.CrossRefGoogle Scholar
Bollani, L et al. (2015) Revised recommendations concerning palivizumab prophylaxis for respiratory syncytial virus (RSV). Italian Journal of Pediatrics 41, 97.CrossRefGoogle Scholar
Simões, EAF et al. (2018) Past, present and future approaches to the prevention and treatment of respiratory syncytial virus infection in children. Infectious Diseases and Therapy 7, 87120.CrossRefGoogle ScholarPubMed
Figueras-Aloy, J et al. (2008) FLIP-2 Study: risk factors linked to respiratory syncytial virus infection requiring hospitalization in premature infants born in Spain at a gestational age of 32 to 35 weeks. Pediatric Infectious Disease Journal 27, 788793.CrossRefGoogle Scholar
Blanken, MO et al. (2013) Prospective validation of a prognostic model for respiratory syncytial virus bronchiolitis in late preterm infants: a multicenter birth cohort study. PLoS ONE 8, e59161.CrossRefGoogle ScholarPubMed
Law, BJ et al. (2004) The Pediatric Investigators Collaborative Network on Infections in Canada study of predictors of hospitalization for respiratory syncytial virus infection for infants born at 33 through 35 completed weeks of gestation. Pediatric Infectious Disease Journal 23, 806814.CrossRefGoogle ScholarPubMed
Sheridan-Pereira, M et al. (2016) Respiratory syncytial virus preterm (32–36 completed weeks of gestation) risk estimation measure for RSV hospitalization in Ireland: a prospective study. Pediatric Infectious Disease Journal 35, 1924.Google ScholarPubMed
Lanari, M et al. (2015) Risk factors for bronchiolitis hospitalization during the first year of life in a multicentre Italian birth cohort. Italian Journal of Pediatrics 41, 40.CrossRefGoogle Scholar
Ambrose, CS et al. (2014) Respiratory syncytial virus disease in preterm infants in the U.S. born at 32–35 weeks gestation not receiving immunoprophylaxis. Pediatric Infectious Disease Journal 33, 576582.CrossRefGoogle Scholar
Straňák, Z et al. (2016) Predictors of RSV LRTI hospitalization in infants born at 33 to 35 weeks gestational age: a large multinational study (PONI). PLoS ONE 11, e0157446.CrossRefGoogle Scholar
Anderson, EJ et al. (2017) Burden of severe respiratory syncytial virus disease among 33–35 weeks’ gestational age infants born during multiple respiratory syncytial virus seasons. Pediatric Infectious Disease Journal 36, 160167.CrossRefGoogle ScholarPubMed
Haerskjold, A et al. (2016) Risk factors for hospitalization for respiratory syncytial virus infection: a population-based cohort study of Danish children. Pediatric Infectious Disease Journal 35, 6165.Google ScholarPubMed
Anderson, EJ et al. (2017) SENTINEL1: an observational study of respiratory syncytial virus hospitalizations among U.S. infants born at 29 to 35 weeks’ gestational age not receiving immunoprophylaxis. American Journal of Perinatology 34, 5161.CrossRefGoogle Scholar
Gijtenbeek, RG et al. (2015) RSV Infection among children born moderately preterm in a community-based cohort. European Journal of Pediatrics 174, 435442.CrossRefGoogle Scholar
Anderson, EJ et al. Effects of timing of birth hospitalization discharge, birth month, and chronologic age on respiratory syncytial virus (RSV) hospitalizations of US preterm infants not receiving immunoprophylaxis. Presented at the Pediatric Academic Societies Meeting (PAS); May 5–8, 2018; Toronto, Canada.Google Scholar
Anderson, EJ et al. (2020) SENTINEL1: two-season study of respiratory syncytial virus hospitalizations among U.S. infants born at 29 to 35 weeks’ gestational age not receiving immunoprophylaxis. American Journal of Perinatology 37, 421429.Google Scholar
Hall, CB et al. (2013) Respiratory syncytial virus-associated hospitalizations among children less than 24 months of age. Pediatrics 132, e341e348.CrossRefGoogle ScholarPubMed
Horn, SD and Smout, RJ (2003) Effect of prematurity on respiratory syncytial virus hospital resource use and outcomes. Journal of Pediatrics 143, S133S141.CrossRefGoogle ScholarPubMed
Langston, C et al. (1984) Human lung growth in late gestation and in the neonate. American Review of Respiratory Disease 129, 607613.Google ScholarPubMed
Friedrich, L et al. (2006) Reduced lung function in healthy preterm infants in the first months of life. American Journal of Respiratory and Critical Care Medicine 173, 442447.CrossRefGoogle ScholarPubMed
Blanken, MO et al. (2018) Cost-effectiveness of rule-based immunoprophylaxis against respiratory syncytial virus infections in preterm infants. European Journal of Pediatrics 177, 133144.CrossRefGoogle ScholarPubMed
Palmer, L et al. (2011) Respiratory outcomes, utilization and costs 12 months following a respiratory syncytial virus diagnosis among commercially insured late-preterm infants. Current Medical Research and Opinion 27, 403412.CrossRefGoogle ScholarPubMed
Sampalis, JS (2003) Morbidity and mortality after RSV-associated hospitalizations among premature Canadian infants. The Journal of Pediatrics 143, S150S156.CrossRefGoogle ScholarPubMed
Blanken, MO et al. (2018) Risk scoring tool to predict respiratory syncytial virus hospitalisation in premature infants. Pediatric Pulmonology 53, 605612.CrossRefGoogle ScholarPubMed
Sánchez Luna, M et al. (2020) Expert consensus on palivizumab use for respiratory syncytial virus in developed countries. Paediatric Respiratory Reviews 33, 3544.CrossRefGoogle Scholar
Figure 0

Table 1. Overview of included studies

Figure 1

Fig. 1. Derivation of pooled dataset.

wGA, weeks' gestational age; *9 cases which were not hospital confirmed, 11 where there was no record of wGA.
Figure 2

Fig. 2. Distribution of RSVH incidence by month*

RSVH, respiratory syncytial virus hospitalisation. *Data from FLIP-2, IBC, PREMI and RISK (studies with year-round data capture). Total RSVHs: 371.
Figure 3

Table 2. Healthcare resource use during RSVH