RCH logo

Clinical Practice Guidelines

Community acquired pneumonia

  • PIC logo
    PIC Endorsed

  • See also

    Parapneumonic effusion                                                      
    Sepsis
    Influenza
    Assessment of severity of respiratory conditions

    Key Points

    1. Community acquired pneumonia (CAP) can be diagnosed clinically and is most often due to viruses
    2. Chest X-Ray (CXR), blood tests and microbiological investigations are not recommended for routine use in the diagnosis and management of CAP
    3. For non-severe pneumonia, high dose oral amoxicillin is recommended, even for inpatient use 
    4. For infants <1 month of age see Recognition of the seriously unwell neonate and young infant and Sepsis guidelines

    Background

    • Pneumonia can be defined clinically as the presence of fever, cough and tachypnoea at rest (and retractions in younger children)
    • “Complicated pneumonia” occurs when there is a complication such as parapneumonic effusion, empyema, lung abscess or necrotising pneumonia 

    Assessment

    History

    • Fever
    • Tachypnoea at rest
    • Cough
    • Increased work of breathing/respiratory distress
    • Apnoea (neonates)
    • Abdominal pain

    Examination

    • Appears lethargic/unwell  
    • Hypoxaemia
    • Tachypnoea
    • Chest wall in-drawing, retractions, grunting, nasal flaring
    • Crackles and/or bronchial breathing on auscultation
    • Absent breath sounds and a dull percussion note suggest a pleural effusion 

    Assessment of severity

    See Assessment of severity of respiratory conditions

    Severe pneumonia should be considered if there are clinical features of pneumonia and one or more of:

    Consider sepsis in children with severe pneumonia

    Management

    Investigations

    Investigations, including CXR, are not recommended routinely for CAP, particularly in those with mild disease who are expected to be managed as an outpatient 

    Chest X-Ray (CXR)

    • Recommended when severe or complicated pneumonia is suspected
    • Consider repeating if the child deteriorates at any time or fails to clinically improve after 48-72 hours of appropriate antibiotic therapy
    • Follow-up CXR is not required for those who have uncomplicated pneumonia or small parapneumonic effusion and recover uneventfully
    • Follow-up CXR is recommended after 6 weeks for:
      • complicated pneumonia
      • recurrent pneumonia involving the same lobe or if initial suspicion of a chest mass, anatomical abnormality or foreign body

    Severe or complicated pneumonia

    • UEC for children receiving intravenous fluids 
    • FBE and blood film 
    • Microbiological investigations 
      • Blood culture
      • Influenza PCR (nasal swab or aspirate)
      • COVID-19 testing (as per local testing criteria)
      • Testing for other viral pathogens will not change management
      • Testing for atypical pathogens is unhelpful as it does not differentiate infection from asymptomatic carriage
    • Acute phase reactants (including CRP and procalcitonin) cannot distinguish between a viral or bacterial cause nor indicate severity
    • Consider sepsis

    Treatment

    Admission to hospital is required for children who require supplemental O2, hydration support with NG or IV fluids, or moderate to severe work of breathing

    • Provide supplemental oxygen if saturations are <90%  
    • If giving NG or IV maintenance fluids, limit fluids to 2/3 of the child’s calculated fluid requirement to avoid fluid overload, with regular clinical review of fluid status
    • Advice regarding antibiotic management is summarised in the algorithm below. High dose oral amoxicillin is as effective as IV benzylpenicillin   
    • Most children, including hospitalised children, can be managed with oral antibiotics 
    • Antimicrobial recommendations may vary according to local antimicrobial susceptibility patterns; please refer tolocal guidelines

      Community acquired pneumonia

    Penicillin hypersensitivity

    Refer to Therapeutic Guidelines and Antibiotic prescribing in children with reported penicillin or cephalosporin allergy for guidance on assessing severity of allergy and appropriate antimicrobial options

    For immediate and/or severe penicillin hypersensitivity, non-beta-lactam antibiotic alternatives for CAP include  

    • Oral
      • Doxycycline 50 mg (<26 kg), 75 mg (26-35 kg), 100 mg (>35 kg) oral BD
      • Azithromycin 10 mg/kg (max 500 mg) oral daily 
    • Intravenous
      • Ciprofloxacin 10 mg/kg (max 400 mg) IV 12 hourly

                   PLUS

      • Vancomycin  IV (see local hospital protocol for doses)

    Atypical pneumonia

    There is no proven benefit from treatment of Mycoplasma pneumoniae pneumonia but it may be considered in severe pneumonia not responding to treatment

    Consider consultation with local paediatric team when

    • Child fulfills criteria for hospital admission
    • Outpatient therapy fails

    Consider transfer when

    • Severe or complicated pneumonia
    • Comorbidities such as cardiac disease, chronic respiratory disease, immune deficiency or suppression are present
    • Child requiring care above the level of comfort of the local hospital

    For emergency advice and paediatric or neonatal ICU transfers, see Retrieval Services

    Consider discharge when

    Child is maintaining adequate oxygenation and oral intake 
    Note: children managed as outpatients should have medical review in 24–48 hrs

    Parent information

    Pneumonia

    Last updated October 2023

  • Reference List

    1. Ambroggio L, Brokamp C, Mantyla R et al. Validation of the British Thoracic Society Severity Criteria for Pediatric Community-acquired Pneumonia. Pediatr Infect Dis J 2019;38:894–899
    2. Ambroggio L. Beta-lactam versus beta- lactam/macrolide therapy in pediatric outpatient pneumonia. Pediatr Pulmonol. 2016 May;51(5):541-8.
    3. Ambroggio L, Test M, Metlay JP, Graf TR, Blosky MA, Macaluso M, Shah SS Comparative Effectiveness of Beta-lactam Versus Macrolide Monotherapy in Children with Pneumonia Diagnosed in the Outpatient Setting. Pediatr Infect Dis J. 2015 Aug;34(8):839-42.
    4. Biondi E, McCulloh R, Alverson B, Klein A, Dixon A, Ralston S. Treatment of mycoplasma pneumonia: a systematic review. Pediatrics. 2014 Jun;133(6):1081-90. doi: 10.1542/peds.2013-3729
    5. Bradley, J.S., Byington, C.L., Shah, S.S. The management of community- acquired pneumonia in infants and children older than 3 months of age: Clinical practice guidelines by the Pediatric Infectious Diseases Society and the Infectious Diseases Society of America. Clin Infect Dis, 2011; 53:e25.
    6. Brendan J McMulla BJ, Andresen D, Blyth CC et al. Antibiotic duration and timing of the switch from intravenous to oral route for bacterial infections in children: systematic review and guidelines. Lancet Infect Dis 2016; 16: e139–52
    7. Chaves GS, Freitas DA, Santino TA, et al. Chest physiotherapy for pneumonia in children. Cochrane Database Syst Rev 2019; 1:CD010277.
    8. Dean P, Florin TA. Factors Associated With Pneumonia Severity in Children: A Systematic Review. Journal of the Pediatric Infectious Diseases Society 2018;7(4):323–34
    9. Fritz CQ, Edwards KM, Self WH, et al. Prevalence, Risk Factors, and Outcomes of Bacteremic Pneumonia in Children. Pediatrics. 2019;144(1):e20183090
    10. Gardiner SJ, Gavranich JB, Chang AB. Antibiotics for community-acquired lower respiratory tract infections secondary to Mycoplasma pneumoniae in children. Cochrane Database Syst Rev. 2015 Jan 8;1:CD004875.
    11. Harris, M., Clark, J., Coote, N. British Thoracic Society guidelines for the management of community acquired pneumonia in children: update 2011. Thorax, 2011; 66:ii1
    12. Jain S, Williams DJ, Arnold SR. Community-Acquired Pneumonia Requiring Hospitalization among U.S. Children. N Engl J Med 2015; 372:835-845 DOI: 10.1056/NEJMoa1405870. Retrieved from: https://www.nejm.org/doi/10.1056/NEJMoa1405870
    13. Lassi ZS, Imdad A, Bhutta ZA. Short-course versus long-course intravenous therapy with the same antibiotic for severe community-acquired pneumonia in children aged two months to 59 months. Cochrane Database Syst Rev 2017; 10:CD008032.
    14. Leyenaar JK, Shieh MS, Lagu T, Pekow PS, Lindenauer P. Comparative effectiveness of ceftriaxone in combination with a macrolide compared with ceftriaxone alone for pediatric patients hospitalized with community-acquired pneumonia. Pediatr Infect Dis J. 2014 Apr;33(4):387-92.
    15. McCrossan P, McNaughten B, Shields M, Thompson A. Is follow up chest X-ray required in children with round pneumonia? Arch Dis Child 2017; 102:1182.
    16. McCulloh, R.J. & Patel, K. Recent Developments in Pediatric Community-Acquired Pneumonia. Curr Infect Dis Rep (2016) 18: 14. https://doi.org/10.1007/s11908-016-0521. Retrieved from: https://link.springer.com/content/pdf/10.1007%2Fs11908-016-0521-1.pdf
    17. Nascimento-Carvalho CM; Madhi SA; O'Brien KL. Review of guidelines for evidence-based management for childhood community- acquired pneumonia in under-5 years from developed and developing countries. Pediatric Infectious Disease Journal. 2013;32(11):1281-2
    18. Shah S, Florin T, Ambroggio L. Procalcitonin in Childhood Pneumonia, Journal of the Pediatric Infectious Diseases Society, 2018;7(1): 54 – 55
    19. Stockmann C, Ampofo K, Killpack J, et al. Procalcitonin Accurately Identifies Hospitalized Children With Low Risk of Bacterial Community-Acquired Pneumonia. J Pediatric Infect Dis Soc. 2018;7(1):46–53. doi:10.1093/jpids/piw091
    20. Williams DJ, Edwards KM, Self WH et al. Effectiveness ofβ-Lactam Monotherapy vs Macrolide Combination Therapy for Children Hospitalized With Pneumonia. JAMA Pediatr. 2017;171(12):1184.
    21. Williams DJ, Zhu Y, Grijalva CG, et al. Predicting Severe Pneumonia Outcomes in Children. Pediatrics. 2016; 138(4):e20161019