Ventilator-Associated Pneumonia

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Ventilator-associated pneumonia (VAP) occurs in patients that have been on mechanical ventilation for more than 48 hours. It presents with clinical signs that include purulent tracheal discharge, fevers, and respiratory distress in the presence of microorganisms. This activity reviews the evaluation and management of ventilator-associated pneumonia and highlights the role of interprofessional team members in collaborating to provide well-coordinated care and enhance outcomes for affected patients.

Objectives:

  • Identify the pathophysiology of ventilator-associated pneumonia.
  • Review the differential diagnosis of ventilator-associated pneumonia.
  • Describe the history and physical exam findings typically seen in patients with ventilator-associated pneumonia.
  • Explain why careful planning and discussion amongst interprofessional team members involved in the management of patients with ventilator-associated pneumonia will improve outcomes.

Introduction

Ventilator-associated pneumonia (VAP) is a term used to describe pneumonia (lung infection) that develops in a patient who has been on mechanical ventilation for more than 48 hours. Ventilator-associated pneumonia is the second most common hospital-acquired infection among pediatrics and neonatal intensive care unit patients. It accounts for 7% to 32% of healthcare-associated infections and 10% of all pediatric device-related infections reported to the National Healthcare Safety Network (NHSN). Generally, the rate of pneumonia in pediatric intensive care units (PICU) is lower than in adult intensive care units (ICU). In neonates, the rate of ventilator-associated pneumonia is inversely proportional to birth weight. There is limited data on infants and children with VAP, so most of the information is extrapolated from adult studies. [1][2][3]

Children with artificial airways, such as a tracheostomy tube for management of chronic respiratory failure or an endotracheal for acute airway management, are at risk for ventilator-associated pneumonia. It is difficult to diagnose ventilator-associated pneumonia in any patient, and this holds true in young children, particularly in the neonatal ICU population. In 2008, the Centers for Disease Control (CDC) and National Healthcare Safety Network (NHSN) have attempted to provide reproducible criteria for the surveillance of ventilator-associated pneumonia. They have classified it as three types: (1) clinically defined, (2) pneumonia with laboratory findings, and (3) pneumonia in immunocompromised patients. Infants and children are usually classified to the first category.

Tracheitis Versus Ventilator-associated Pneumonia

Ventilator-associated pneumonia is part of a spectrum of upper airway infection after the of an artificial airway with bacteria. For convenience, the infection of an artificial airway after colonization is either diagnosed as tracheitis or ventilator-associated pneumonia. 

  • Tracheitis is the presence of clinical signs of purulent tracheal discharge, fevers, respiratory distress, and the presence of bacteria and white blood cells in the tracheal aspirate without radiological signs of pneumonia.

  • Ventilator-associated pneumonia includes clinical signs of purulent tracheal discharge, fevers, respiratory distress, and micro-biological signs of the presence of microorganisms along with white blood cells in the tracheal aspirate along with radiological evidence of pneumonia.

Etiology

Ventilator-associated pneumonia is typically bacterial and from a single organism. However polymicrobial infections are increasing. In a large retrospective review done in the ICU settings of three hospitals, the microbiology was the same across adult and pediatric hospitals. The most common organisms were Staphylococcus aureus (28.4 %), Pseudomonas aeruginosa (25.2 %), and other gram negatives (26.6%). [4][5]

Artificial airways become colonized with pathogenic bacteria soon after intubation or tracheostomy, and the major pathogens include both gram-positive and gram-negative bacteria: S. aureus (including MRSA), P. aeruginosa, and Klebsiella and Enterobacter species. Patients in a NICU have a risk of Enterococcus species and group B Streptococcus as well. Other pathogens include the Streptococcus, Enterobacteriaceae, and Acinetobacter species. Anaerobic bacteria are an uncommon cause of Ventilator-associated pneumonia but can play a role in polymicrobial infections, particularly when pneumonia is due to aspiration.  Nosocomial viruses and fungi are rare causes of pneumonia in immunocompetent hosts.

In addition, early pneumonia (less than 4 days after admission to the hospital) is most likely from antibiotic-sensitive community-acquired organisms, and late pneumonia (more than 4 days) is more likely due to antibiotic-resistant organisms. However, this distinction is not helpful in children who are frequently admitted to the hospital.

Epidemiology

Pediatric patients seem to have a lower risk of ventilator-associated pneumonia than adults, possibly due to fewer comorbidities. According to NHSN, 304 participating hospitals revealed ventilator-associated pneumonia rates of 2.36 to 2.08 per 1000 device-days among neonates weighing less than 750 grams and between 750 and 1,000 grams, respectively.[6][7]

The estimated incidence of ventilator-associated infection in pediatric ICU ranges from 1.8 to 8.3 per 1000 ventilator days.

Pathophysiology

There are few mechanisms suggested for development of ventilator-associated pneumonia: (1) most commonly it is thought to be a progression from colonization of the upper airway, leading to tracheal colonization, then tracheitis, and finally pneumonia. This depends on the number, type, and virulence of the bacteria as well as natural host defenses such as mechanical factors and humoral and cellular immunity. Mechanical defenses, such as ciliary motion and mucus secretion, can be altered in an intubated patient. Artificial airway inhibits gag reflex and ciliary functions and provides a substrate for growth of biofilm which acts as a reservoir for pathogens. This biofilm can be dislodged and delivered to the lower respiratory tract through mechanical suctioning or high-pressure airflow, leading to pneumonia in a susceptible host. Bacteria overgrowth can be secondary to proton-pump inhibitors and histamine type 2 receptor antagonists for stress ulcer prophylaxis, which neutralized gastric pH and promotes colonization of the upper gastrointestinal tract. In a supine patient with likely depressed mental status (possibly secondary to sedation), the risk of aspiration is high.[8]

History and Physical

Diagnosis of ventilator-associated pneumonia can be difficult. It requires a combination of clinical, radiographic, and microbiologic data. The longer the length of intubation, the higher the likelihood of ventilator-associated pneumonia. Ventilator-associated pneumonia is suspected in the setting of fever, change in auscultation exam, a change in the chest x-ray, and an increasing requirement for respiratory support. However, auscultation is hindered by sounds of the ventilation system itself, especially with high-frequency ventilation. Many neonates have chest x-ray findings that interfere with the early detection of new infiltrates. 

Evaluation

Clinical findings include fever, leukocytosis or leukopenia, purulent secretions, and worsening gas exchange. Chest X-ray with new or worsening pulmonary infiltrates, cavitation, air bronchograms, or pneumatoceles is a requirement. Microbiologic data are important, both for diagnosis and for guiding treatment. Samples of lower respiratory tract secretions are often obtained and sent for culture as well as blood cultures in all patients suspected of ventilator-associated pneumonia. However, many experts recommend against taking a culture from intubated patients as most are colonized after 48 hours, and the culture is of little clinical use.[9][10][11]

In adults, specimens are obtained via bronchoscopy, lung biopsy, lung aspiration, protected specimen brushing (PSB), or transtracheal aspiration rather than by aspiration of tracheal content through an endotracheal tube.  However, use of bronchoscopic bronchoalveolar lavage (BAL) or PSB to obtain secretions of the lower respiratory tract for quantitative bacterial culture is limited in children due to technical difficulties and potential for complication.  This problem is even more challenging in NICU patients. 

Obtaining a microbiological specimen from neonates is often impossible, so the CDC has come up with purely clinical criteria for the diagnosis of ventilator-associated pneumonia among infants less than one year of age. These include

  • Worsening gas exchange as evident by oxygen desaturations,
  • Increased oxygen requirements,
  • Increased ventilator demand and
  • Three of the seven following findings: temperature instability, leukopenia or leukocytosis and left shift, new onset of purulent sputum or change in sputum character or increased respiratory secretions or increased suctioning requirements, apnea, tachypnea, nasal flaring with retraction of chest wall or nasal flaring with grunting, wheezing, rales or rhonchi, cough, bradycardia, or tachycardia.

Treatment / Management

Once ventilator-associated pneumonia is suspected and appropriate culture samples are sent, empirical therapy will be based on the duration of intubation and hospitalization, prior or current antibiotic therapy, the severity of clinical disease, and knowledge of local pathogen’s susceptibility patterns. Initial broad-spectrum therapy with coverage of gram-negative bacilli, including P. aeruginosa, and possibly methicillin-resistant S. aureus is generally appropriate. Treatment is then narrowed based on subsequent culture data and clinical and radiographic findings.[12][13][14]

Treatment duration has not been evaluated in children. In adults, uncomplicated cases may be treated with 7 to 10 days of therapy. For complicated cases or those with necrotizing pneumonia, at least 14 days of therapy should be administered. Courses less than 7 days may be appropriate for children with ventilator-associated tracheitis without evidence of pneumonia.

Differential Diagnosis

  • Aspiration pneumonia
  • Virus or bacterial pneumonia
  • Pneumocystis jirovecii pneumonia
  • Heart failure

Complications

  • Stress ulcers
  • Deep vein thrombosis
  • Multiorgan failure

Consultations

Pediatric infectious disease and pediatric pulmonology consultations should be considered in such cases.

Pearls and Other Issues

  • Summary of risk factors for ventilator-associated pneumonia and the area of focus for prevention include: (1) treatment factors that promote colonization of oropharynx or stomach, (2) factors that promote gastric reflux and aspiration like depressed mental status, supine position, nasogastric tubes, (3) duration of intubation and mechanical ventilation, and (4) factors that interfere with adequate pulmonary toilet, thoracic or abdominal surgery or immobilization. 
  • Methods for decreasing the incidence of ventilator-associated pneumonia include but are not limited to the following, and most institutions utilize “prevention bundles” to reduce the risk: (1) judicious use of reflux medications, (2) removal of unnecessary nasogastric tubes, and (3) daily evaluation of readiness to extubate, pain-control, and maintenance of mechanical ventilation system are all part of protocols ICUs use to decrease the rate of ventilator-associated pneumonia.

Enhancing Healthcare Team Outcomes

Ventilator-associated pneumonia is usually managed by an interprofessional team that includes an intensivist, pulmonologist, respiratory therapy, ICU nurse, dietitian, pharmacist, and thoracic surgeon. The key with VAP is to reduce the risk by enforcing preventive techniques in patient care. All the modifiable risk factors should be addressed such as endotracheal and tracheostomy suctioning, use of gastric acid modifying agents, enteral nutrition, hand washing and single use of equipment. The supine position should be avoided, and one should minimize transport of the patient in and out of the ICU. The cuff pressure of the endotracheal tube should be at 20 mmHg or above, to help prevent passage of oropharyngeal contents into the lower airways. The pharmacist should ensure that the right antibiotics are selected and that there is a recycling of the medications to avoid the development of resistant organisms. The patient must be fed enterally whenever possible. Finally, there should be protocols for weaning and early extubation in order to avoid VAP.[15][16] (Level V)

Outcomes

In general, VAP is associated with a higher mortality when the patient has numerous comorbidities. However, younger patients with no additional organ involvement do tend to have a good prognosis without any major sequelae. Higher mortality rates have been reported in older patients, diabetics, those with COPD, smokers and poor functional status.[17][18] (Level V)


(Click Image to Enlarge)
<p>Ventilator-Associated Aspiration Pneumonia. Chest radiograph showing ventilator-associated aspiration pneumonia.</p>

Ventilator-Associated Aspiration Pneumonia. Chest radiograph showing ventilator-associated aspiration pneumonia.


Melvil, Public Domain, via Wikimedia Commons
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GoleNaz A. Kohbodi

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Venkat Rajasurya

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Asif Noor

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References

[1]

Semenkovich TR, Frederiksen C, Hudson JL, Subramanian M, Kollef MH, Patterson GA, Kreisel D, Meyers BF, Kozower BD, Puri V. Postoperative Pneumonia Prevention in Pulmonary Resections: A Feasibility Pilot Study. The Annals of thoracic surgery. 2019 Jan:107(1):262-270. doi: 10.1016/j.athoracsur.2018.08.008. Epub 2018 Oct 3     [PubMed PMID: 30291834]

Level 2 (mid-level) evidence

[2]

Silva ARAD, Silva TCD, Bom GJT, Vasconcelos RMB, Junior RS. Ventilator-associated pneumonia agents in Brazilian Neonatal Intensive Care Units - a systematic review. The Brazilian journal of infectious diseases : an official publication of the Brazilian Society of Infectious Diseases. 2018 Jul-Aug:22(4):338-344. doi: 10.1016/j.bjid.2018.06.002. Epub 2018 Jul 5     [PubMed PMID: 30278872]

Level 1 (high-level) evidence

[3]

Antcliffe DB, Wolfer AM, O'Dea KP, Takata M, Holmes E, Gordon AC. Profiling inflammatory markers in patients with pneumonia on intensive care. Scientific reports. 2018 Oct 3:8(1):14736. doi: 10.1038/s41598-018-32938-6. Epub 2018 Oct 3     [PubMed PMID: 30283005]

[4]

Jain V, Vashisht R, Yilmaz G, Bhardwaj A. Pneumonia Pathology. StatPearls. 2023 Jan:():     [PubMed PMID: 30252372]

[5]

Iosifidis E, Pitsava G, Roilides E. Ventilator-associated pneumonia in neonates and children: a systematic analysis of diagnostic methods and prevention. Future microbiology. 2018 Sep:13():1431-1446. doi: 10.2217/fmb-2018-0108. Epub 2018 Sep 26     [PubMed PMID: 30256161]

Level 1 (high-level) evidence

[6]

Watson K, Heales LJ, Fernando J, Reoch J, Tan E, Smith K, Austin D, Divanoglou A. Incidence and characteristics of ventilator-associated pneumonia in a regional non-tertiary Australian intensive care unit: protocol for a retrospective clinical audit study. BMJ open. 2018 Sep 8:8(9):e021733. doi: 10.1136/bmjopen-2018-021733. Epub 2018 Sep 8     [PubMed PMID: 30196266]

Level 2 (mid-level) evidence

[7]

Ferrer M, Torres A. Epidemiology of ICU-acquired pneumonia. Current opinion in critical care. 2018 Oct:24(5):325-331. doi: 10.1097/MCC.0000000000000536. Epub     [PubMed PMID: 30080701]

Level 3 (low-level) evidence

[8]

Phillips-Houlbracq M, Ricard JD, Foucrier A, Yoder-Himes D, Gaudry S, Bex J, Messika J, Margetis D, Chatel J, Dobrindt U, Denamur E, Roux D. Pathophysiology of Escherichia coli pneumonia: Respective contribution of pathogenicity islands to virulence. International journal of medical microbiology : IJMM. 2018 Mar:308(2):290-296. doi: 10.1016/j.ijmm.2018.01.003. Epub 2018 Jan 5     [PubMed PMID: 29325882]

[9]

Grief SN, Loza JK. Guidelines for the Evaluation and Treatment of Pneumonia. Primary care. 2018 Sep:45(3):485-503. doi: 10.1016/j.pop.2018.04.001. Epub     [PubMed PMID: 30115336]

[10]

Dianti M, Luna CM. Do we need biomarkers for the follow-up and shortening of antibiotic treatment duration? Current opinion in critical care. 2018 Oct:24(5):361-369. doi: 10.1097/MCC.0000000000000540. Epub     [PubMed PMID: 30124483]

Level 3 (low-level) evidence

[11]

Ambaras Khan R, Aziz Z. The methodological quality of guidelines for hospital-acquired pneumonia and ventilator-associated pneumonia: A systematic review. Journal of clinical pharmacy and therapeutics. 2018 Aug:43(4):450-459. doi: 10.1111/jcpt.12696. Epub 2018 May 2     [PubMed PMID: 29722052]

Level 2 (mid-level) evidence

[12]

Chomton M, Brossier D, Sauthier M, Vallières E, Dubois J, Emeriaud G, Jouvet P. Ventilator-Associated Pneumonia and Events in Pediatric Intensive Care: A Single Center Study. Pediatric critical care medicine : a journal of the Society of Critical Care Medicine and the World Federation of Pediatric Intensive and Critical Care Societies. 2018 Dec:19(12):1106-1113. doi: 10.1097/PCC.0000000000001720. Epub     [PubMed PMID: 30234676]

[13]

Martin-Loeches I, Rodriguez AH, Torres A. New guidelines for hospital-acquired pneumonia/ventilator-associated pneumonia: USA vs. Europe. Current opinion in critical care. 2018 Oct:24(5):347-352. doi: 10.1097/MCC.0000000000000535. Epub     [PubMed PMID: 30063491]

Level 3 (low-level) evidence

[14]

Niederman MS. Antibiotic treatment of hospital-acquired pneumonia: is it different from ventilator-associated pneumonia? Current opinion in critical care. 2018 Oct:24(5):353-360. doi: 10.1097/MCC.0000000000000531. Epub     [PubMed PMID: 30028739]

Level 3 (low-level) evidence

[15]

Jam R, Mesquida J, Hernández Ó, Sandalinas I, Turégano C, Carrillo E, Pedragosa R, Valls J, Parera A, Ateca B, Salamero M, Jane R, Oliva JC, Delgado-Hito P. Nursing workload and compliance with non-pharmacological measures to prevent ventilator-associated pneumonia: a multicentre study. Nursing in critical care. 2018 Nov:23(6):291-298. doi: 10.1111/nicc.12380. Epub 2018 Sep 5     [PubMed PMID: 30182383]

[16]

Munro S, Haile-Mariam A, Greenwell C, Demirci S, Farooqi O, Vasudeva S. Implementation and Dissemination of a Department of Veterans Affairs Oral Care Initiative to Prevent Hospital-Acquired Pneumonia Among Nonventilated Patients. Nursing administration quarterly. 2018 Oct/Dec:42(4):363-372. doi: 10.1097/NAQ.0000000000000308. Epub     [PubMed PMID: 30180083]

Level 2 (mid-level) evidence

[17]

Chen Z, Shi X. Adverse events of high-dose tigecycline in the treatment of ventilator-associated pneumonia due to multidrug-resistant pathogens. Medicine. 2018 Sep:97(38):e12467. doi: 10.1097/MD.0000000000012467. Epub     [PubMed PMID: 30235740]

[18]

Pozuelo-Carrascosa DP, Torres-Costoso A, Alvarez-Bueno C, Cavero-Redondo I, López Muñoz P, Martínez-Vizcaíno V. Multimodality respiratory physiotherapy reduces mortality but may not prevent ventilator-associated pneumonia or reduce length of stay in the intensive care unit: a systematic review. Journal of physiotherapy. 2018 Oct:64(4):222-228. doi: 10.1016/j.jphys.2018.08.005. Epub 2018 Sep 13     [PubMed PMID: 30220625]

Level 1 (high-level) evidence