- 1Child Health Division, Menzies School of Health Research, Charles Darwin University, Darwin, NT, Australia
- 2Department of Paediatrics, Royal Darwin Hospital, Darwin, NT, Australia
- 3Menzies Health Institute Queensland, Griffith University and Gold Coast University Hospital, Gold Coast, QLD, Australia
- 4Department of Paediatrics, Townsville Hospital, Townsville, QLD, Australia
- 5Queensland Paediatric Infectious Diseases Laboratory, Queensland Children’s Medical Research Institute, Sir Albert Sakzewski Virus Research Centre, Children’s Health Queensland Hospital and Health Service, University of Queensland, Herston, QLD, Australia
- 6Clinical Medical Virology Centre, School of Chemistry and Molecular Biosciences, University of Queensland, St Lucia, QLD, Australia
- 7The University of Auckland and Starship Children’s Hospital, Auckland, New Zealand
- 8Queensland Children’s Medical Research Institute, Children’s Health Queensland, Queensland University of Technology, Brisbane, QLD, Australia
Background: Bronchiolitis is a major health burden in infants globally, particularly among Indigenous populations. It is unknown if 3 weeks of azithromycin improve clinical outcomes beyond the hospitalization period. In an international, double-blind randomized controlled trial, we determined if 3 weeks of azithromycin improved clinical outcomes in Indigenous infants hospitalized with bronchiolitis.
Methods: Infants aged ≤24 months were enrolled from three centers and randomized to receive three once-weekly doses of either azithromycin (30 mg/kg) or placebo. Nasopharyngeal swabs were collected at baseline and 48 h later. Primary endpoints were hospital length of stay (LOS) and duration of oxygen supplementation monitored every 12 h until judged ready for discharge. Secondary outcomes were: day-21 symptom/signs, respiratory rehospitalizations within 6 months post-discharge and impact upon nasopharyngeal bacteria and virus shedding at 48 h.
Results: Two hundred nineteen infants were randomized (n = 106 azithromycin, n = 113 placebo). No significant between-group differences were found for LOS (median 54 h for each group, difference = 0 h, 95% CI: −6, 8; p = 0.8), time receiving oxygen (azithromycin = 40 h, placebo = 35 h, group difference = 5 h, 95% CI: −8, 11; p = 0.7), day-21 symptom/signs, or rehospitalization within 6 months (azithromycin n = 31, placebo n = 25 infants, p = 0.2). Azithromycin reduced nasopharyngeal bacterial carriage (between-group difference 0.4 bacteria/child, 95% CI: 0.2, 0.6; p < 0.001), but had no significant effect upon virus detection rates.
Conclusion: Despite reducing nasopharyngeal bacterial carriage, three large once-weekly doses of azithromycin did not confer any benefit over placebo during the bronchiolitis illness or 6 months post hospitalization. Azithromycin should not be used routinely to treat infants hospitalized with bronchiolitis.
Clinical trial registration: The trial was registered with the Australian and New Zealand Clinical Trials Register: Clinical trials number: ACTRN1261000036099.
Introduction
Bronchiolitis is the most common acute viral lower respiratory infection in infants worldwide causing more than three million hospitalizations annually (1). Indigenous children from affluent countries, such as Australia and New Zealand, are at particular risk. They are more likely than non-Indigenous children to be hospitalized (2, 3), to have longer hospital stays (2), to receive antibiotics for pneumonia (2, 4), and to be rehospitalized in the next 6 months with a respiratory illness (5). Indigenous children also have high rates of pneumonia and bronchiectasis (the latter related to recurrent pneumonia) (6, 7) and their upper airways are colonized with bacterial pathogens from an early age (8).
Supportive care, including supplemental oxygen, respiratory support, and fluid replacement, underpins bronchiolitis management. Clinical trials have shown bronchodilators, mucolytics, anti-viral, and anti-inflammatory agents to be ineffective (9). However, macrolide antibiotics pose as an attractive alternative, especially for Indigenous infants with their high risk of severe disease and secondary bacterial complications (5). In addition to possessing direct antibacterial actions, including activity against Mycoplasma pneumoniae and Chlamydiales species, macrolides modulate macrophage, neutrophil, and epithelial cell function in vitro and in experimental models (10), and possess potential anti-viral properties. Clarithromycin reduces respiratory syncytial virus (RSV) receptor numbers on epithelial cell surfaces; while azithromycin induces interferon-stimulated genes in rhinovirus (RV)-infected bronchial epithelial cells (11, 12). Finally, a single azithromycin dose decreases nasopharyngeal bacterial loads (5) and transiently reduces the risk of acute lower respiratory infections in African children following mass trachoma prevention campaigns or when contributing to combination therapy for malaria (13, 14).
Four placebo, double-blind, randomized controlled trials (RCTs) have evaluated the efficacy of macrolides in children hospitalized with bronchiolitis (5, 15–17). The first trial from Turkey (15), involving 21 infants aged ≤7 months with RSV, found that clarithromycin daily for 3 weeks significantly reduced hospital length of stay (LOS) and supplemental oxygen and intravenous fluid requirements compared to placebo. In contrast, 3 later RCTs (5, 16, 17) involving a total of 352 infants (up to age 2 years) with clinically diagnosed bronchiolitis from Australia, the Netherlands, and Brazil failed to demonstrate any clinical benefit using azithromycin for 1, 3, or 7 days, respectively. The Turkish trial was also the only one where treatment extended beyond the period in hospital where just 1 of the 12 infants in the clarithromycin group was re-hospitalized compared with 4 of 9 receiving placebo (15).
At the time we started our study, only the RCTs from Turkey (15) and the Netherlands (16) had been completed. We believed Indigenous infants were more like high-risk children in Turkey and might also benefit from a longer treatment course (the Turkish study was the only one to have addressed this question) (15). This is of considerable importance for Indigenous infants where respiratory symptoms and recurrent hospitalized respiratory illnesses are major risk factors for developing bronchiectasis (5–7). As administering twice-daily clarithromycin on an ambulatory basis is impractical in our setting (18), we took advantage of azithromycin’s long half-life and favorable pharmacokinetics by opting to determine whether a longer course (three large once-weekly doses) of azithromycin for Indigenous infants hospitalized with bronchiolitis improved clinical outcomes (LOS and duration of oxygen supplementation). Secondary aims were to: (i) determine the effects of azithromycin on respiratory symptoms and signs at day-21 and respiratory hospitalizations in the following 6-month period; (ii) assess the short-term impact of azithromycin upon nasopharyngeal carriage and respiratory virus shedding and; (iii) describe the viruses, M. pneumoniae and Chlamydiales species detected in these infants.
Materials and Methods
Study Design and Setting
This was a multi-center, randomized, double-blind, placebo-controlled trial. Infants were recruited at the Royal Darwin (June 2010–September 2013) and Townsville Hospitals (August 2010–June 2013), Australia and the Auckland Starship Children’s Hospital (November 2012–September 2013), New Zealand. Human Research Ethics Committees at all participating institutions approved the study and caregivers provided written, informed consent. The study was registered with the Australian and New Zealand Clinical Trials Register: ACTRN12608000150347 and monitored by an independent data safety monitoring board (DSMB).
Participants
As described in detail previously (19), eligible infants were aged ≤24 months and hospitalized with a standardized clinical diagnosis of bronchiolitis (age-adjusted tachypnea with wheeze or crackles), had parent-ascribed Indigenous ethnicity (Australian Aboriginal, Torres Strait Islander, Maori, and/or Pacific Islander), were consented within 24 h of hospitalization and had caregivers with a mobile phone (see supplement for exclusion criteria and tachypnea definitions).
Randomization, Allocation and Blinding, and Medications
An independent statistician used a computer-generated, permuted block design to generate randomization sequences. Sealed opaque envelopes (selecting one of the eight different bottle codes) concealed the treatment allocation. Infants were allocated in a 1:1 ratio, stratified by age (≤6 or >6 months), oxygen supplementation on presentation (yes/no) and site (Darwin, Townsville, or Auckland), to once-weekly doses of oral azithromycin or placebo for 3 weeks. Neither the study team (researchers, hospital staff) nor parents were aware of assigned treatment groups until data analysis was completed.
The first dose was given in the hospital (30 mg/kg azithromycin or equal volume of placebo). The remaining two doses were supervised directly by study nurses (urban-based participants) or given at home by caregivers (remote-based participants) at weekly intervals. Study nurses contacted families via mobile phones to help ensure adherence (20).
Clinical Assessment, Management, and Outcomes
Demographic, medical history, and clinical data were recorded on standardized data collection forms. A validated severity score was employed (see Supplementary Material). Infants with bronchiolitis were managed at each site according to a common protocol, which outlined when supplementary oxygen was indicated (SpO2 <94%) and when nasogastric feeds or intravenous fluids were required. The protocol was in place for several months before commencing the trial. Infants received additional therapies (other than macrolides) at the discretion of the treating pediatrician.
The primary endpoints of LOS for respiratory illness and duration of oxygen requirement (where applicable) were monitored every 12 h. LOS was the time from admission to time “ready for discharge” from respiratory care as defined by SpO2 >94% in air for >16 h and feeding adequately. In our setting, “ready for discharge” from respiratory care can differ from LOS, as discharge from hospital may be delayed because of non-medical factors (such as waiting for air transport back to remote communities). For the other clinical outcomes, the day-21 review was conducted by study nurses (urban-based participants) and local health clinic staff (remote-based). Respiratory rehospitalization within 6 months of discharge was recorded through community and hospital electronic records. Adverse events were monitored daily in hospital by research staff and following discharge with weekly phone calls until the day-21 review.
Specimen Collection and Processing
Nasopharyngeal swabs (NPS) taken before initial study medications were administered and repeated 48 h later, and were processed as described previously (21–23) for viruses and atypical bacteria (C. pneumoniae, Simkania negevensis, M. pneumoniae) using real-time polymerase chain reaction (PCR) assays (see Supplementary Material for list of viruses). NPS were cultured for respiratory bacterial pathogens that also underwent antibiotic susceptibility testing (24).
Sample Size and Analysis
Based upon our previous data where the mean LOS in Indigenous infants with bronchiolitis was 96 (SD 24) hours (2), we estimated a total sample of 200 infants (100 in each age sub-group: ≤6 months and >6 months) would provide 94% power to detect a difference in the mean LOS of 12 h between treatment groups at the 5% significance level (two-tailed) and 95% power to detect a reduction in respiratory rehospitalization within the next 6 months from 30 to 10% (19).
Data were analyzed according to our published protocol. Data were analyzed according to the group the child was allocated to. Only available data were analyzed. Between-group differences were tested using Fisher’s exact test (for proportions) and Mann–Whitney U test (for continuous variables). A 95% confidence interval (CI) was obtained for the difference in medians between treatment groups (25). Subgroup analysis was performed by age (≤6 and >6 months) as planned (19), and also for groups based on oxygen requirement when enrolled, remoteness, antibiotic use, and previous respiratory hospitalizations for the three clinical outcomes. These post hoc subgroup analyses were conducted that might inform clinical practice. p-Values are reported for the subgroup × treatment interaction term in a linear regression model (for log-transformed LOS and duration of supplemental oxygen) and in a logistic regression model (for any readmissions within 6 months) with main effects for just treatment group and subgroup. Data were also analyzed adjusting for significant between-group differences at baseline.
Results
We recruited 219 infants (106 randomized to azithromycin, 113 to placebo (Figure 1). Overall, 218 received dose-1 in hospital; 102 (azithromycin) and 111 (placebo) received dose-2 and 94 (azithromycin); and 106 (placebo) received dose-3.
Demographical and clinical characteristics were similar between treatment groups, apart from household smoke exposure involving more infants in the azithromycin (69%) than the placebo (50%) group, p = 0.01; see Table 1). Of the study cohort, 133 (61%) required oxygen during hospitalization. Non-macrolide antibiotics were prescribed in 93 (43%) infants before hospitalization (see Supplementary Material) and none received steroids or required intensive care management. Thirty-eight infants were hospitalized previously for a respiratory illness (azithromycin: 18; placebo: 20). Retention was high (≥97%) for the clinical endpoint at day-21.
Table 1. Demographic and clinical characteristics of 219 patients randomized to treatment with either azithromycin (n = 106) or placebo (n = 113).
Clinical Outcomes
No significant between-group differences were found for LOS or duration of supplemental oxygen (Figures 2A,B). The median LOS of 54 h was identical in both groups (difference = 0 h, 95% CI: −6, 8; p = 0.8), while the median time receiving oxygen was 40 h in the azithromycin group and 35 h in the placebo group (difference = 5 h, 95% CI: −8, 11; p = 0.7).
Figure 2. (A) Length of hospital stay (LOS) until ready for discharge from respiratory care. There was no significant difference between children randomized to azithromycin and placebo. (B) Time children received supplementary oxygen (where applicable). There was no significant difference between children randomized to azithromycin and placebo.
Day-21 Clinical Review and 6-Month Readmission
Two hundred ten (97%) infants completed the day-21 review (Figure 1). Although persistent symptoms or signs were more common in placebo group, the between-group differences were not significant (Table 2).
Overall, 81 (azithromycin n = 47, placebo n = 34) respiratory rehospitalizations were recorded from 56 participants (azithromycin n = 31, placebo n = 25). No significant between-group differences were found (odds ratio for any hospitalization 1.5, 95% CI: 0.8, 3.0, p = 0.2). Sixty (74%) rehospitalizations were for wheezing-associated illness.
There was no evidence of a differential effect of azithromycin on any of the main three clinical outcomes for any of the subgroups (see Tables S2–S4 in Supplementary Material). Adjustment for household smoking exposure had negligible effect on the trial’s main analyses (see Table S5 in Supplementary Material).
Microbiology
Nasopharyngeal swabs were collected from 217 infants at baseline and 215 at 48 h. At baseline, at least 1 virus was detected in 174 (81%) infants (see Figure S1 in Supplementary Material). RSV was detected in 91 (42%), followed by HRV (79; 37%) and adenovirus (14; 7%). The mean number of viruses detected per infant hardly changed from baseline to 48 h; azithromycin: 1.0–0.9 viruses (difference 0.1, 95%CI: −0.2, 0.2; p = 0.4); placebo: 1.1–1.0 viruses (difference 0.1, 95%CI: −0.02, 0.3; p = 0.09).
Nasopharyngeal swabs isolations of S. pneumoniae, non-typable H. influenzae, and M. catarrhalis at 48 h were less common in the azithromycin group than in the placebo group (Table 3). On average, there were 0.4 (95% CI: 0.2, 0.6; p < 0.001) fewer bacterial species per infant in the azithromycin group.
Adverse Events
Three adverse events were reported to our DSMB. In the azithromycin group, one infant presented to hospital with vomiting and diarrhea and another vomited the trial medication. In the placebo group, one infant presented to hospital with wheezing and a rash. All recovered and none discontinued the trial.
Discussion
This is the first international, multicentre, double-blind RCT of an extended course of macrolides in bronchiolitis. In this study involving 219 Indigenous infants, we found that three once-weekly doses of azithromycin (compared to placebo), conferred no benefit in terms of LOS, duration of oxygen supplementation, day-21 symptom/signs, or respiratory rehospitalizations within 6 months post discharge. Azithromycin significantly reduced the mean number of nasopharyngeal bacteria per infant, but not the mean number of viruses per infant.
Our study is larger than the four preceding published studies on macrolides in bronchiolitis (5, 15–17) and involved a group of infants from populations at high risk for chronic suppurative lung disease (6). Our findings on the lack of beneficial effect of azithromycin for hospital-based outcomes (LOS and duration of oxygen supplementation) are concordant with three of these studies (5, 16, 17). To date, the Turkish study is unique (15) where 3 weeks of clarithromycin reported reduced LOS, oxygen supplementation, and respiratory rehospitalization within the following 6 months. Possible reasons for the difference between the Turkish (15) and other studies (5, 16, 17) include: using clarithromycin with its greater lung penetration and potential anti-RSV activity (11), differences in sample size, attrition population characteristics, the role of chance, and increased risk of bias associated with small studies.
We used a longer course of azithromycin than the other studies (5, 15–17) and did not find any clinically significant between-group outcomes. Azithromycin had no significant effect on the presence of persistent symptoms/signs on day-21 review and the proportion with persistent respiratory symptoms or signs (14–24%) are similar to another report of 25% infants remaining symptomatic after 21 days (26). Furthermore, the importance of the symptoms beyond hospitalization of persistent cough and wheeze was highlighted in a guideline on bronchiolitis (27).
The proportion of respiratory rehospitalizations within 6 months of discharge (25%) was also similar to other trials (5, 15). Rehospitalization for respiratory illness is an important outcome because it is an independent risk factor for bronchiectasis in Indigenous children (6). We targeted this high-risk group, as respiratory diseases are prevalent and more severe and persistent in this population (5, 28).
The mean number of nasopharyngeal respiratory bacteria was reduced more in the azithromycin than the placebo arm, as seen in our previous short-term RCT (5). Although the number of macrolide-resistant bacteria at 48 h also declined, this was not to the same extent as found in susceptible strains. Meanwhile, detection rates for respiratory viruses between treatment groups changed little over the 48 h following enrollment, though PCR detects nucleic acids, it is not possible to determine whether differences in viable viruses existed with azithromycin treatment.
Our study has several other limitations, which may have resulted in the negative results of our RCT. First, including an older age group increased the risk of including those with asthma. However, our cohort’s median age of 6 months (IQR 3, 9) reduced this possibility. Further, in both the UK and USA bronchiolitis guidelines, the upper age limit is 23–24 months. Second, in the Australian centers, we included those hospitalized previously for an acute respiratory infection, which may have contributed to the number of respiratory rehospitalizations (27, 29). Third, the concurrent use of antibiotics in two-thirds of infants with bronchiolitis may limit the ability of additional macrolide treatment to improve outcomes. We were unable to influence the clinical practice of physicians on this matter. However, subgroup analyses on previous respiratory hospitalization, or antibiotic use did not show any significant differences on any of our outcomes (see Supplementary Material). Fourth, our strategy of using three large once-weekly azithromycin doses may have produced sub-optimal results. This, however, is unlikely as prior RCTs of daily azithromycin found no benefit (16, 17). Moreover, in children, single large doses of azithromycin can successfully treat otitis media (18), while for several weeks after its mass distribution within rural African villages for controlling trachoma, azithromycin reduced the risk of acute lower respiratory infections by more than one-third (13). Although our RCT (18) used the same regime for long-term therapy of children with bronchiectasis and showed that azithromycin significantly reduced the exacerbation rate by 50% (compared to placebo), the different disease and younger age group in this RCT meant an alternative dose and/or regime for optimal efficacy may have been required. Finally, even though parents reported verbally that doses-2 and 3 were given, we were unable to directly observe these for remote-based infants (n = 145). However, the day-21 follow-up rate of >97% at the local health clinic implies that parents are likely to have adhered to the study protocol. This is supported by feedback from research nurses who interviewed parents throughout the trial.
Our study was aimed at infants at high risk of future bronchiectasis and employed a 3-week equivalent course in a multicentre setting. This design was to maximize the chances of demonstrating a clinical benefit for azithromycin in our target population, by reducing subsequent hospitalization and shortening hospital stay (both are independent risk factors for later development of bronchiectasis). Despite this, no advantage from receiving azithromycin was identified. Moreover, there are now growing concerns over the increasing global consumption of antibiotics and rising rates of antibiotic resistance, especially when few new anti-microbial agents are in the developmental pipeline (30, 31). Much of this antibiotic resistance is being driven by antibiotics prescribed for viral respiratory infections, most notably long-acting, broad-spectrum agents, including azithromycin (32, 33). An emerging fear for this young age group is that antibiotics may also adversely affect the developing intestinal “microbiome” with potential deleterious long-term effects upon gastrointestinal, immunological, and metabolic programing (34). Thus, given our study’s negative findings and the concerns over the association between azithromycin and increased carriage of macrolide-resistant pathogens (35), the increasing need for anti-microbial stewardship, potential immediate and long-term adverse events, and associated costs, it is clear that these factors outweigh any postulated, but still unproven benefits of macrolides in this patient population.
Conclusion
In this RCT of Indigenous infants hospitalized with bronchiolitis, we found that three once-weekly doses of azithromycin significantly reduced nasopharyngeal bacterial carriage, but did not have any significant impact on viruses or short (reduced LOS or duration of oxygen supplementation) or long-term (decreased odds of persistent symptoms at day-21 or respiratory rehospitalization within 6 months of discharge) clinical benefits compared with placebo. In light of these results, similar findings in other studies, and fears over rising antibiotic resistance, azithromycin should not be used to treat infants hospitalized with viral bronchiolitis.
Author Contributions
GM set up and managed the study, recruited participants, performed the data analysis, and drafted the manuscript. AC conceptualized the study. AC and KG co-drafted the manuscript. AC, PM, KG, TS, AW, IM co-designed the study and contributed to obtaining the grant, interpreted the data, and edited the manuscript. CB was responsible for overseeing all aspects of the trial in NZ. CM, AW, and CB were responsible for standardizing the management of bronchiolitis in their units, recruiting participants, and edited the manuscript. CM, LV, NJ, CM were responsible for recruiting participants and edited the manuscript. TS and IM assisted in the viral components of the study and edited the manuscript. HS-V assisted in the microbiological components of the study and edited the manuscript. MC assisted in the data analysis and edited the manuscript. All authors read and approved the final manuscript.
Conflict of Interest Statement
The authors declare that they have no conflicts of interest relevant to this article to disclose. This study was funded by National Health and Medical Research Council (NHMRC) grants (605809) and supported by a Centre for Research Excellence in Lung Health of Aboriginal and Torres Strait Islander Children (1040830). Gabrielle B. McCallum is supported by a NHMRC scholarship (1055262); Anne B. Chang is funded by a NHMRC practitioner fellowship (545216 and 1058213). Heidi Smith-Vaughan is supported by a NHMRC Career Development Fellowship (1024175).
Acknowledgments
We thank Louise Axford-Haines for assisting in data collection, Kim Hare, Vanya Hampton, Donna Woltring, Chris Wevill, Yuku Ruzsicska, Jemima Beissbarth, Jane Gaydon, and Rebecca Rockett for processing the viral and bacterial samples. We also thank the DSMB for their guidance throughout the trial (Dr. Kerry Ann O’Grady, Dr. William Frishman, Prof. Alan Isles, A/Prof. Alan Ruben, Ms. Linda Ward). We thank the Indigenous Reference Group (http://www.menzies.edu.au/page/About_Us/Board_and_Menzies_committees/Indigenous_Reference_Group/), for their advice and support through this trial, in Australia, and the Kaiatawhai and the Pacific Island Family Support in New Zealand. We thank the medical and nursing staff for their ongoing support and identifying the children for the study, including the General Pediatric Teams at Starship Children’s Hospital. We are grateful for all the children and families who participated in the study.
Author Note
Protocol: a full study protocol can be accessed at www.trialsjournal.com “Randomized controlled trial of azithromycin to reduce the morbidity of bronchiolitis in Indigenous infants: a protocol.”
Supplementary Material
The Supplementary Material for this article can be found online at http://journal.frontiersin.org/article/10.3389/fped.2015.00032
Abbreviations
CI, confidence interval; DSMB, data safety monitoring board; HRV, human rhinovirus; LOS, length of stay; NHMRC, National Health and Medical Research Council; NPS, nasopharyngeal swab; PCR, polymerase chain reaction; RCT, randomized controlled trial; RSV, respiratory syncytial virus.
References
1. Nair H, Nokes DJ, Gessner BD, Dherani M, Madhi SA, Singleton RJ, et al. Global burden of acute lower respiratory infections due to respiratory syncytial virus in young children: a systematic review and meta-analysis. Lancet (2010) 375:1545–55. doi: 10.1016/S0140-6736(10)60206-1
Pubmed Abstract | Pubmed Full Text | CrossRef Full Text | Google Scholar
2. Bailey EJ, Maclennan C, Morris PS, Kruske SG, Brown N, Chang AB. Risks of severity and readmission of Indigenous and non-Indigenous children hospitalised for bronchiolitis. J Paediatr Child Health (2009) 45:593–7. doi:10.1111/j.1440-1754.2009.01571.x
Pubmed Abstract | Pubmed Full Text | CrossRef Full Text | Google Scholar
3. Grimwood K, Cohet C, Rich FJ, Cheng S, Wood C, Redshaw N, et al. Risk factors for respiratory syncytial virus bronchiolitis hospital admission in New Zealand. Epidemiol Infect (2008) 136:1333–41. doi:10.1017/S0950268807000180
Pubmed Abstract | Pubmed Full Text | CrossRef Full Text | Google Scholar
4. Vogel AM, Lennon DR, Harding JE, Pinnock RE, Graham DA, Grimwood K, et al. Variations in bronchiolitis management between five new Zealand hospitals: can we do better? J Paediatr Child Health (2003) 39:40–5. doi:10.1046/j.1440-1754.2003.00069.x
Pubmed Abstract | Pubmed Full Text | CrossRef Full Text | Google Scholar
5. McCallum GB, Morris PS, Chatfield MD, Maclennan C, White AV, Sloots TP, et al. A single dose of azithromycin does not improve clinical outcomes of children hospitalised with bronchiolitis: a randomised, placebo-controlled trial. PLoS One (2013) 8:e74316. doi:10.1371/journal.pone.0074316
Pubmed Abstract | Pubmed Full Text | CrossRef Full Text | Google Scholar
6. Singleton RJ, Valery PC, Morris P, Byrnes CA, Grimwood K, Redding G, et al. Indigenous children from three countries with non-cystic fibrosis chronic suppurative lung disease/bronchiectasis. Pediatr Pulmonol (2014) 49:189–200. doi:10.1002/ppul.22763
Pubmed Abstract | Pubmed Full Text | CrossRef Full Text | Google Scholar
7. Valery PC, Torzillo PJ, Mulholland K, Boyce NC, Purdie DM, Chang AB. Hospital-based case-control study of bronchiectasis in Indigenous children in central Australia. Pediatr Infect Dis J (2004) 23:902–8. doi:10.1097/01.inf.0000142508.33623.2f
Pubmed Abstract | Pubmed Full Text | CrossRef Full Text | Google Scholar
8. Leach AJ, Boswell JB, Asche V, Nienhuys TG, Mathews JD. Bacterial-colonization of the nasopharynx predicts very early-onset and persistence of otitis-media in Australian aboriginal infants. Pediatr Infect Dis J (1994) 13:983–9. doi:10.1097/00006454-199411000-00009
Pubmed Abstract | Pubmed Full Text | CrossRef Full Text | Google Scholar
9. Schroeder AR, Mansbach JM. Recent evidence on the management of bronchiolitis. Curr Opin Pediatr (2014) 26:328–33. doi:10.1097/MOP.0000000000000090
Pubmed Abstract | Pubmed Full Text | CrossRef Full Text | Google Scholar
10. Parnham MJ, Erakovic Haber V, Giamarellos-Bourboulis EJ, Perletti G, Verleden GM, Vos R. Azithromycin: mechanisms of action and their relevance for clinical applications. Pharmacol Ther (2014) 143:225–45. doi:10.1016/j.pharmthera.2014.03.003
Pubmed Abstract | Pubmed Full Text | CrossRef Full Text | Google Scholar
11. Asada M, Yoshida M, Suzuki T, Hatachi Y, Sasaki T, Yasuda H, et al. Macrolide antibiotics inhibit respiratory syncytial virus infection in human airway epithelial cells. Antiviral Res (2009) 83:191–200. doi:10.1016/j.antiviral.2009.05.003
Pubmed Abstract | Pubmed Full Text | CrossRef Full Text | Google Scholar
12. Gielen V, Johnston SL, Edwards MR. Azithromycin induces anti-viral responses in bronchial epithelial cells. Eur Respir J (2010) 36:646–54. doi:10.1183/09031936.00095809
Pubmed Abstract | Pubmed Full Text | CrossRef Full Text | Google Scholar
13. Coles CL, Levens J, Seidman JC, Mkocha H, Munoz B, West S. Mass distribution of azithromycin for trachoma control is associated with short-term reduction in risk of acute lower respiratory infection in young children. Pediatr Infect Dis J (2012) 31:341–6. doi:10.1097/INF.0b013e31824155c9
Pubmed Abstract | Pubmed Full Text | CrossRef Full Text | Google Scholar
14. Gilliams EA, Jumare J, Claassen CW, Thesing PC, Nyirenda OM, Dzinjalamala FK, et al. Chloroquine-azithromycin combination antimalarial treatment decreases risk of respiratory- and gastrointestinal-tract infections in Malawian children. J Infect Dis (2014) 210:585–92. doi:10.1093/infdis/jiu171
Pubmed Abstract | Pubmed Full Text | CrossRef Full Text | Google Scholar
15. Tahan F, Ozcan A, Koc N. Clarithromycin in the treatment of Rsv bronchiolitis: a double-blind, randomised, placebo-controlled trial. Eur Respir J (2007) 29:91–7. doi:10.1183/09031936.00029206
Pubmed Abstract | Pubmed Full Text | CrossRef Full Text | Google Scholar
16. Kneyber MC, van Woensel JB, Uijtendaal E, Uiterwaal CS, Kimpen JL. Azithromycin does not improve disease course in hospitalized infants with respiratory syncytial virus (Rsv) lower respiratory tract disease: a randomized equivalence trial. Pediatr Pulmonol (2008) 43:142–9. doi:10.1002/ppul.20748
Pubmed Abstract | Pubmed Full Text | CrossRef Full Text | Google Scholar
17. Pinto LA, Pitrez PM, Luisi F, de Mello PP, Gerhardt M, Ferlini R, et al. Azithromycin therapy in hospitalized infants with acute bronchiolitis is not associated with better clinical outcomes: a randomized, double-blinded, and placebo-controlled clinical trial. J Pediatr (2012) 161:1104–8. doi:10.1016/j.jpeds.2012.05.053
Pubmed Abstract | Pubmed Full Text | CrossRef Full Text | Google Scholar
18. Valery PC, Morris PS, Byrnes CA, Grimwood K, Torzillo PJ, Bauert PA, et al. Long-term azithromycin for Indigenous children with non-cystic-fibrosis bronchiectasis or chronic suppurative lung disease (bronchiectasis intervention study): a multicentre, double-blind, randomised controlled trial. Lancet Respir Med (2013) 1:610–20. doi:10.1016/S2213-2600(13)70185-1
Pubmed Abstract | Pubmed Full Text | CrossRef Full Text | Google Scholar
19. Chang AB, Grimwood K, White AV, Maclennan C, Sloots TP, Sive A, et al. Randomized placebo-controlled trial on azithromycin to reduce the morbidity of bronchiolitis in Indigenous Australian infants: rationale and protocol. Trials (2011) 12:94. doi:10.1186/1745-6215-12-94
Pubmed Abstract | Pubmed Full Text | CrossRef Full Text | Google Scholar
20. McCallum GB, Versteegh LA, Morris PS, McKay CC, Jacobsen NJ, White AV, et al. Mobile phones support adherence and retention of Indigenous participants in a randomised controlled trial: strategies and lessons learnt. BMC Public Health (2014) 14:622. doi:10.1186/1471-2458-14-622
Pubmed Abstract | Pubmed Full Text | CrossRef Full Text | Google Scholar
21. Stubbs E, Hare K, Wilson C, Morris P, Leach AJ. Streptococcus pneumoniae and noncapsular Haemophilus Influenzae nasal carriage and hand contamination in children – a comparison of two populations at risk of otitis media. Pediatr Infect Dis J (2005) 24:423–8. doi:10.1097/01.inf.0000160945.87356.ca
Pubmed Abstract | Pubmed Full Text | CrossRef Full Text | Google Scholar
22. Hare KM, Grimwood K, Leach AJ, Smith-Vaughan H, Torzillo PJ, Morris PS, et al. Respiratory bacterial pathogens in the nasopharynx and lower airways of Australian Indigenous children with bronchiectasis. J Pediatr (2010) 157:1001–5. doi:10.1016/j.jpeds.2010.06.002
Pubmed Abstract | Pubmed Full Text | CrossRef Full Text | Google Scholar
23. Lambert SB, Ware RS, Cook AL, Maguire FA, Whiley DM, Bialasiewicz S, et al. Observational research in childhood infectious diseases (orchid): a dynamic birth cohort study. BMJ Open (2012) 2:e002134. doi:10.1136/bmjopen-2012-002134
Pubmed Abstract | Pubmed Full Text | CrossRef Full Text | Google Scholar
24. Hare KM, Leach AJ, Morris PS, Smith-Vaughan H, Torzillo P, Bauert P, et al. Impact of recent antibiotics on nasopharyngeal carriage and lower airway infection in Indigenous Australian children with non-cystic fibrosis bronchiectasis. Int J Antimicrob Agents (2012) 40:365–9. doi:10.1016/j.ijantimicag.2012.05.018
Pubmed Abstract | Pubmed Full Text | CrossRef Full Text | Google Scholar
25. Altman Douglas MD. Bryant Trevor, Gardner Stephen. Statistics with Confidence. Bristol: BMJ Books (1989). p. 74–9.
26. Petruzella FD, Gorelick MH. Duration of illness in infants with bronchiolitis evaluated in the emergency department. Pediatrics (2010) 126:285–90. doi:10.1542/peds.2009-2189
27. Baumer JH. Sign guideline on bronchiolitis in infants. Arch Dis Child Educ Pract Ed (2007) 92:e149–51. doi:10.1136/adc.2007.126524
28. Trenholme AA, Byrnes CA, McBride C, Lennon DR, Chan-Mow F, Vogel AM, et al. Respiratory health outcomes 1 year after admission with severe lower respiratory tract infection. Pediatr Pulmonol (2013) 48:772–9. doi:10.1002/ppul.22661
Pubmed Abstract | Pubmed Full Text | CrossRef Full Text | Google Scholar
29. Ralston SL, Lieberthal AS, Meissner HC, Alverson BK, Baley JE, Gadomski AM, et al. Clinical practice guideline: the diagnosis, management, and prevention of bronchiolitis. Pediatrics (2014) 134:e1474–502. doi:10.1542/peds.2014-2742
Pubmed Abstract | Pubmed Full Text | CrossRef Full Text | Google Scholar
30. Laxminarayan R, Duse A, Wattal C, Zaidi AK, Wertheim HF, Sumpradit N, et al. Antibiotic resistance-the need for global solutions. Lancet Infect Dis (2013) 13:1057–98. doi:10.1016/S1473-3099(13)70318-9
Pubmed Abstract | Pubmed Full Text | CrossRef Full Text | Google Scholar
31. Van Boeckel TP, Gandra S, Ashok A, Caudron Q, Grenfell BT, Levin SA, et al. Global antibiotic consumption 2000 to 2010: an analysis of national pharmaceutical sales data. Lancet Infect Dis (2014) 14:742–50. doi:10.1016/S1473-3099(14)70780-7
Pubmed Abstract | Pubmed Full Text | CrossRef Full Text | Google Scholar
32. Young M, Chopra M, Ojoo A. Antibiotic effectiveness and child survival. Lancet Infect Dis (2013) 13:1004–5. doi:10.1016/S1473-3099(13)70317-7
33. Lynch JP III, Zhanel GG. Streptococcus pneumoniae: epidemiology and risk factors, evolution of antimicrobial resistance, and impact of vaccines. Curr Opin Pulm Med (2010) 16:217–25. doi:10.1097/MCP.0b013e3283385653
Pubmed Abstract | Pubmed Full Text | CrossRef Full Text | Google Scholar
34. Houghteling PD, Walker WA. Why is initial bacterial colonization of the intestine important to infants’ and children’s health? J Pediatr Gastroenterol Nutr (2015) 60:294–307. doi:10.1097/MPG.0000000000000597
Pubmed Abstract | Pubmed Full Text | CrossRef Full Text | Google Scholar
35. Hare KM, Singleton RJ, Grimwood K, Valery PC, Cheng AC, Morris PS, et al. Longitudinal nasopharyngeal carriage and antibiotic resistance of respiratory bacteria in Indigenous Australian and Alaska native children with bronchiectasis. PLoS One (2013) 8:e70478. doi:10.1371/journal.pone.0070478
Pubmed Abstract | Pubmed Full Text | CrossRef Full Text | Google Scholar
Keywords: bronchiolitis, Indigenous, viruses, bacteria, respiratory syncytial virus, macrolides, azithromycin, randomized controlled trial
Citation: McCallum GB, Morris PS, Grimwood K, Maclennan C, White AV, Chatfield MD, Sloots TP, Mackay IM, Smith-Vaughan H, McKay CC, Versteegh LA, Jacobsen N, Mobberley C, Byrnes CA and Chang AB (2015) Three-weekly doses of azithromycin for Indigenous infants hospitalized with bronchiolitis: a multicentre, randomized, placebo-controlled trial. Front. Pediatr. 3:32. doi: 10.3389/fped.2015.00032
Received: 04 March 2015; Paper pending published: 21 March 2015;
Accepted: 05 April 2015; Published: 21 April 2015
Edited by:
Malcolm King, Canadian Institutes of Health Research, CanadaReviewed by:
Yusei Ohshima, University of Fukui, JapanLarry C. Lands, Montreal Children’s Hospital – McGill University Health Centre, Canada
Copyright: © 2015 McCallum, Morris, Grimwood, Maclennan, White, Chatfield, Sloots, Mackay, Smith-Vaughan, McKay, Versteegh, Jacobsen, Mobberley, Byrnes and Chang. This is an open-access article distributed under the terms of the Creative Commons Attribution License (CC BY). The use, distribution or reproduction in other forums is permitted, provided the original author(s) or licensor are credited and that the original publication in this journal is cited, in accordance with accepted academic practice. No use, distribution or reproduction is permitted which does not comply with these terms.
*Correspondence: Gabrielle B. McCallum, Menzies School of Health Research, John Mathews Building, Building 58, Royal Darwin Hospital Campus, Rocklands Drive, Casuarina, NT 0811, Australia gabrielle.mccallum@menzies.edu.au