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Haemophilus Influenzae
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Haemophilus influenzae can cause serious invasive disease especially in young children. Invasive disease is usually caused by encapsulated strains of the organism. Six typeable capsular serotypes (a-f) are known to cause disease; non-typeable encapsulated strains can occasionally cause invasive disease.
- The most virulent strain is H. influenzae type b (Hib), which accounts for more than 95% of H. influenzae infections in children and half of infections in adults. Hib may cause bacteremia, meningitis, cellulitis, epiglottitis, septic arthritis, pneumonia, and pleural or gallbladder empyema.
- Less common Hib infections include endophthalmitis, urinary tract infection, abscesses, cervical adenitis, glossitis, osteomyelitis, and endocarditis.
- Non-encapsulated and non-typeable, H. influenzae strains cause mucosal infections, including exacerbations of chronic bronchitis,1 otitis media, conjunctivitis, sinusitis, bronchitis, and pneumonia.
Risk factors
- Hib bacteria are carried in the nose and throat without showing any signs of infection. Hib is spread through coughing, sneezing or close contact with an infected person.
- Before Hib vaccine was introduced, about four in every 100 preschool children carried the Hib organism; after the vaccine was introduced, carriage rates fell below the level of detection.2
- Hib infections are uncommon in patients older than 6 years. However the frequency of Hib infections is increased in patients with asplenia, splenectomy, sickle cell disease, malignancies, and congenital or acquired immunodeficiencies.
- The most common presentation (60% of all cases) of invasive Hib disease is meningitis, frequently accompanied by bacteraemia. Hib meningitis primarily affects children younger than 2 years, with a peak frequency rate occurring in infants aged 6-9 months.
- Fifteen per cent of cases present with epiglottitis. Epiglottitis most commonly occurs in children aged 2-7 years but can also occur in adults.
- Bacteraemia, without any other concomitant infection, occurs in 10% of cases. The remainder is made up of cases of septic arthritis, osteomyelitis, cellulitis, pneumonia and pericarditis.
- Hib pneumonia typically occurs in children aged 4 months to 4 years.
- Hib causes septic arthritis and cellulitis in children younger than 2 years. Hib septic arthritis manifests in adults as well.
- Neonatal infection:
- Often due to non-typeable H. influenzae, which colonises on the maternal genital tract.
- Infection is associated with premature birth, premature rupture of membranes, low birth weight, and maternal chorioamnionitis.
- Presentations include meningitis, pneumonia, respiratory distress, scalp abscess, conjunctivitis, and vesicular eruption.
- Gram stain: small, Gram-negative, pleomorphic coccobacilli with polymorphonuclear cells.
- Bacterial or other relevant body fluid culture: is the most confirmatory method of establishing the diagnosis.
- Slide agglutination with type-specific antisera is used for serotyping H. influenzae.
- Detection of the PRP polysaccharide capsule: methods include countercurrent immunoelectrophoresis and enzyme-linked immunosorbent assay; important for providing a rapid diagnosis. Not affected by prior antibiotics.
- CSF features in meningitis: pleocytosis with a predominance of neutrophils, decreased CSF glucose levels, increased CSF protein, detectable capsular antigen in 90%, and a positive CSF Gram stain result in 80%.
- CT scan: may be required, particularly to identify a possible subdural effusion, in patients with meningitis to exclude raised intracranial pressure, if there are focal neurological findings or failure of expected improvement with appropriate antibiotics.
- Chest x-ray: Hib pneumonia tends to cause more pleural and pericardial involvement compared with other bacterial pneumonias. Community-acquired pneumonias due to non-typeable H. influenzae are characterised by alveolar infiltrates in patchy or lobar distributions.
- Other investigations will depend on the site of infection, e.g. echocardiogram if pericarditis is suspected, joint aspiration for septic arthritis.
- H. influenzae epiglottitis: intravenous cefotaxime or chloramphenicol.
- Exacerbations of chronic bronchitis: amoxicillin, tetracycline or erythromycin; some H. influenzae strains are tetracycline-resistant and 15% of H. influenzae strains are resistant to amoxicillin.
- Meningitis: cefotaxime - treat for at least 10 days; use chloramphenicol instead if there is a history of anaphylaxis to penicillin or to cephalosporins or if organism resistant to cefotaxime; dexamethasone may also be required; give rifampicin for 4 days before hospital discharge.
- The sequelae following Hib meningitis may include deafness, convulsions and intellectual impairment.
- Between 8 and 11% of children who develop Hib meningitis will develop permanent neurological sequelae.4
- The case fatality ratio from Hib meningitis is 4 to 5%.4
- The mortality rate for epiglottitis is 5-10% (due to acute respiratory tract obstruction).
- The mortality rate for neonatal H. influenzae disease is 55%.
Hib immunisation
- Prevents infection in the vaccinated individual and reduces carriage and thus reduces chance of infection in those not vaccinated.5
- Apart from being part of the UK childhood vaccination programme, it is also indicated for those at risk: asplenia, sickle-cell disease, and malignancy.
- Hib vaccines are made from capsular polysaccharide that has been extracted from cultures of Hib bacteria.
- DTaP/IPV/Hib is recommended for all children from two months up to ten years of age.
- Although one dose of Hib vaccine is effective from one year of age, three doses of DTaP/IPV/Hib should be given in order to be fully protected against diphtheria, tetanus, pertussis and polio.
- If the primary course is interrupted it should be resumed but not repeated, allowing an interval of one month between the remaining doses.
Prevention of secondary case of H. influenzae type b disease
- Prophylactic antibiotics should be given to close contacts of patients who have invasive Hib disease.
- Adults: rifampicin 600 mg once daily for 4 days
- Child 1–3 months 10 mg/kg once daily for 4 days: over 3 months 20 mg/kg once daily for 4 days (max. 600 mg daily)
Document references
- Leanord A, Williams C; Haemophilus influenzae in acute exacerbations of chronic obstructive pulmonary disease. Int J Antimicrob Agents. 2002 May;19(5):371-5. [abstract]
- McVernon J, Howard AJ, Slack MP, et al; Long-term impact of vaccination on Haemophilus influenzae type b (Hib) carriage in the United Kingdom. Epidemiol Infect. 2004 Aug;132(4):765-7. [abstract]
- BNF; Section 5.1; Antibacterial drugs.
- Tudor-Williams G, Frankland J, Isaacs D, et al; Haemophilus influenzae type b disease in the Oxford region. Arch Dis Child. 1989 Apr;64(4):517-9. [abstract]
- Swingler G, Fransman D, Hussey G; Conjugate vaccines for preventing Haemophilus influenzae type B infections. Cochrane Database Syst Rev. 2007 Apr 18;(2):CD001729. [abstract]
Internet and further reading
- Health Protection Agency; Haemophilus influenzae type B (Hib).
- Todar's Online Textbook of Bacteriology; Haemophilus influenzae. 2004.
- Devarajan VR; Haemophilus Influenzae Infections. eMedicine, January 2007.
DocID: 2222
Document Version: 20
DocRef: bgp417
Last Updated: 10 Mar 2008
Review Date: 10 Mar 2010
The authors and editors of this article are employed to create accurate and up to date content reflecting reliable research evidence, guidance and best clinical practice. They are free from any commercial conflicts of interest. Find out more about updating.
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