Coxiella burnetii

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Coxiella burnetii /
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Coxiella burnetti

Summary

History

  • Originally described in Australia in 1935 among workers at a meatworks
  • Q fever, for query fever, because the doctor suspected a new infection

Microbiology

  • Highly pleomorphic, intracellular, spore-forming, Gram-negative coccobacillus that causes Q fever
    • Enters cell passively
  • Phase variation, with two phases that differ in their lipopolysaccharides and some other characteristics
    • Phase I: state in nature
  • Related to rickettsiae

Epidemiology

  • Zoonotic disease, most commonly of cattle, sheep, and goats
    • Also infected peripartum cats
    • Maintained in a transmission cycle with ticks or other arthropods
    • Ungulates often asymptomatic
    • Can be detected in air up to 2 weeks post-partum and in soil for 6 months
  • Released by an infected animal during childbirth, though windborne spread can carry it at least 10 km
    • Placenta has an extremely high burden of bacteria
    • Can also be found in stool, urine, and milk
    • Unpasteurized milk
  • Inhaled by humans with an incubation period of 20 days (1 to 39 days)
    • Dose-dependent incubation period
    • Chronic Q fever can be up to 6 months
  • Worldwide distribution, except New Zealand
    • Hepatitis more in Europe, pneumonia more in US

Risk Factors

  • Working with or near animals, especially peripartum
  • Lab exposure
  • Unpasteurized milk

Pathophysiology

  • Bacteria enter lungs, where they proliferate in the macrophages and invade the bloodstream
    • Lives in the phagolysosome
    • Can cause graulomas
  • Alternatively, can enter via tick bite or via ingestion
  • Invasion of bloodstream causes systemic symptoms, with severity depending on the dose inhaled
  • QPH1 is a more virulent strain

Syndromes

  • Can present as asymptomatic, self-limited febrile illness lasting 2 to 14 days (most common), pneumonia, or hepatitis
    • Asymptomatic more common in pregnant women and children
  • Infective endocarditis, osteomyelitis, CNS infection including aseptic meningitis
  • Q fever in immunocompromised host, Q fever in infancy, Q fever in pregnancy
  • Post-Q fever fatigue syndrome

Acute Q fever

  • Fever is uniform finding in all syndromes
  • Chills, headache (severe), fatigue, and myalgias that lasts 2-21 days (14)
  • Can present with rash including urticaria
  • Palpable purpura can be seen in chronic Q fever (that is, endocarditis)

Pneumonia

  • Can present as an atypical pneumonia, a rapidly-progressing pneumonia, and an incidental pneumonia in a febrile patient (most common)
  • A community-acquired pneumonia that doesn't respond to first-line antibiotics (like Legionella and pneumonic tularemia)
  • Cough, though often not present, can be non-productive, productive, or bloody
  • More common in Americas than Europe

Hepatitis

  • Three forms:
    • An infectious hepatitis–like picture
    • Fever of unknown origin, with characteristic granulomas ("donut-like") on liver biopsy
    • An incidental finding in a patient with acute Q fever pneumonia
  • More common in Europe and Americas

CNS infections

  • Can cause Miller-Fischer variant of Guillain-Barré syndrome

Endocarditis

  • Subacute or chronic febrile illess
  • Clubbing and hepatosplenomegaly are common
  • Higher titres are more convincing ≥1:6400

Diagnosis

  • Not readily culturable (nor should you try), though you can see it with Giemsa stain
  • PCR is possible though not common
  • Causes a false-positive RF, APLA
  • Main method of detection is serology

Serology

  • Immunofluorescence assay is standard; no need for EIA
  • Two phases of IgG antibodies (phase I and II)
    • Phase II corresponds more to acute
      • Positive if IgM >50 and IgG >200, or if there's a 4x rise in either titres
      • Detectable by 2 weeks, should be positive by 4
      • Peak at 2 months, then decrease except the IgG in cases of endocarditis
      • Also IgA, but not clinically relevant
    • Phase I corresponds more to chronic
      • Can test for IgG (useful) and IgA (useless) titres
      • IgG ≥ 800 consistent with chronic infection, and is one of the minor Duke criteria for endocarditis
      • IgG ≥ 6400 is suggestive of endovascular infection or endocarditis (major criteria),
  • Two ways to diagnose acute infection
    • Retrospectively with a fourfold rise in both titres from acute to chronic stage, or
    • One-time phase II IgM >50 and IgG >2000
  • Chronic infection is diagnosed clinically, with a phase I IgG titre greater than the phase II IgG titre, and both are at least IgG titre >1:1600
  • IgM antibodies are usually undetectable by 4 months, though IgG may persist for more than a decade

Management

  • Acute Q fever
    • Consider screening for bicuspid valve with TTE if high risk, or baseline TTE
    • Doxycyxline 100mg po bid x 10-14 days
    • Second-line is fluoroquinolones or macrolides
    • Consider monitoring titres for some period afterwards
    • In patients with prosthetic heart valves, consider prolonged treatment as per chronic Q fever (like 1 year)
  • Chronic Q fever
    • Definitely screen for endocarditis
    • Doxycycline + hydroxychloroquine 200mg/d continued until phase I IgG titres have decreased to ≤1:800
      • Hydroxychloroquine potentiates doxycycline in the phagolysosomes (makes the doxy bactericidal)
      • Monitor for ophthalmologic complications, and both have photosensitivity
      • Can adjust dose of hydroxychloroquine to target serum level 0.8 to 1.2 mcg/mL
    • Duration 1.5 years for native valve endocarditis, 2 years for prosthetic valve endocarditis
    • Measure titres every 3-6 months during treatment, then every 3 months for 2 years after completing treatment

Considerations in Pregnancy

  • Coxiella loves the placenta
  • It can be a cause of flu-like illness in pregnanct women with a potential exposure history
    • This can be associated with first-trimester pregnancy loss
  • Doxycycline and fluoroquinolones are contraindicated
  • Septra 1600/320 daily, make sure they're on folic acid supplementation
    • Continue it for the duration of pregnancy
    • Theoretic risk of hyperbilirubinemia in third trimester, so may consider holding it towards the end unless there's documented chronic infection
  • High risk of developing chronic infection, so titres should be monitored for at least 2 years
    • If persistent IgG > 800, consider TEE

Prevention

  • Vaccinate high-risk workers