TRAVEL MEDICINE

Leptospirosis

May 29, 2024 / No Comments

Introduction

  • Leptospirosis: Infectious disorder of animals and humans, most common zoonotic infection globally.
  • Transmission: Through infected animal urine, contaminated soil, or water.
  • Disease Severity: Ranges from a self-limiting flu-like illness to Weil’s disease, which can cause multiorgan failure and death.
  • Occupational Risk: Sewage workers, agricultural workers.
  • Recreational Risk: Water sports enthusiasts.

Etiology

  • Causative Agent: Spirochete bacterium Leptospira.
  • Transmission:
    • Direct contact with urine of infected animals.
    • Contact with contaminated soil or water.

High-Risk Groups

  • Common Animal Vectors: Cattle, pigs, horses, raccoons, porcupines, domesticated dogs.
  • Animal Carriers: Over 160 species can carry the disease without symptoms and act as vectors for months.

Leptospirosis in Australia

Sources of Infection:

  • Occupational Exposure:
    • Livestock and dairy farmers.
    • Abattoir and meat workers.
    • Banana workers (exposure to rodents).
  • Recreational Exposure:
    • Activities like white water rafting, kayaking, ecotourism, and other outdoor activities.
  • International Travel:
    • Travel to tropical, developing countries increases risk for both occupational and recreational exposure.

Environmental and Climatic Factors:

  • Tropical Climates:
    • Ideal conditions for Leptospira survival.
    • Transmission exacerbated by high rainfall and flooding.
  • Poor Sanitation and Drainage:
    • Increases exposure, especially in urban slums with an abundance of rodents.
  • Notable Post-Flooding Outbreaks:
    • Densely populated developing countries such as Brazil, India, and the Philippines.

Pathophysiology, Clinical Features, and Complications

  • Incubation Period: Typically 5 to 14 days, but can range from 2 to 30 days.
  • Entry: Through nonintact skin, mucous membranes, or inhalation of contaminated water.
  • Environmental Survival:
    • Freshwater: up to 16 days.
    • Soil: up to 24 days.
  • Transmission During Pregnancy: Can lead to miscarriage or stillbirth.
  • Spread in Body: Through lymphatics and bloodstream, settling in liver and kidneys.

Biphasic Illness:

  • Acute/Bacteraemic Phase:
    • Duration: 7 to 10 days from symptom onset.
    • Symptoms: Sudden onset of fever, myalgia, headache, calf tenderness, conjunctival suffusion.
    • Non-specific symptoms: Anorexia, nausea, vomiting, abdominal pain, dizziness, lethargy, arthralgia, eye pain, photophobia, rashes.
  • Late/Immune Phase:
    • Onset: >7 days from symptom onset.
    • Symptoms: Immunologically mediated organ damage.
    • Severe Complications: Acute renal failure, pulmonary haemorrhage, myocarditis, arrhythmias, shock, liver failure, coagulopathy, neurological complications.
    • Weil’s Disease:
      • Classic triad of
        • jaundice
        • renal failure
        • haemorrhage
      • not always occurring together
      • High mortality if untreated.
      • Complications: Disseminated intravascular coagulation, haemolytic uraemic syndrome, thrombotic thrombocytopenic purpura.

Neurological Complications:

  • Aseptic meningitis, encephalitis, convulsions.
  • Guillain–Barré syndrome, transverse myelitis, other neurological syndromes.

Ocular Manifestations:

  • Acute or chronic optic complications.
  • Subconjunctival and retinal haemorrhages.
  • Optic neuritis, chronic uveitis.

Differential Diagnosis

  • Viral upper respiratory infections
  • Dengue fever
  • Malaria
  • Hantavirus
  • Hemorrhagic fevers
  • Typhoid fever
  • Cholecystitis
  • Mononucleosis
  • Primary HIV
  • Measles, rubella

Laboratory Diagnosis of Leptospirosis

  • Acute/Bacteraemic Phase:
    • Tests to order:
      • PCR (Polymerase Chain Reaction):
        • Collect blood in a serum-separating tube before starting antibiotics.
        • High sensitivity in the early phase, useful for immediate clinical management.
      • IgM ELISA (Immunoglobulin M Enzyme-Linked Immunosorbent Assay):
        • Lower sensitivity compared to PCR in the early phase but helpful in determining illness phase.
      • Blood Cultures:
        • Use specific culture medium (Ellinghausen–McCullough–Johnson–Harris medium) if available.
        • Cultures examined for six weeks by dark-field microscopy.
  • Late/Immune Phase:
    • Tests to order:
      • IgM ELISA:
        • Reactive results sent to reference laboratories for confirmation by MAT.
      • MAT (Microscopic Agglutination Test):
        • Convalescent sample collected 14 days later to confirm rising titres.
        • Includes a panel of serovars from different serogroups.
  • Case Definition of Leptospirosis (NNDSS):
    • Confirmed Case:
      • Isolation of pathogenic Leptospira species.
      • Fourfold or greater rise in Leptospira MAT titre between acute and convalescent-phase sera.
      • Single Leptospira MAT titre ≥400, supported by a positive ELISA IgM result.
    • Probable Case:
      • Positive IgM ELISA or positive PCR alone.

Additional Investigations Based on Clinical Presentation

  • Full Blood Count:
    • Findings: Leucocytosis, neutrophilia with left shift, lymphopenia, normochromic anaemia, thrombocytopenia.
  • Urea, Electrolytes, Creatinine:
    • Findings: Raised urea and creatinine if renal impairment, low sodium, normal or low potassium (high potassium indicates poor outcomes).
  • Liver Function Tests:
    • Findings: Raised bilirubin (mainly direct), normal or raised liver enzymes, AST and ALT typically three to five times above normal.
  • Urinalysis:
    • Findings: Proteinuria, microscopic haematuria, pyuria, granular casts.
  • Creatine Phosphokinase:
    • Findings: Raised in patients with myalgia.
  • Coagulation:
    • Findings: Raised prothrombin time, partial thromboplastin time, and INR due to impaired liver function.
  • Arterial Blood Gases:
    • Findings: Low PaO2, SaO2, PaO2/FiO2 ratio, metabolic acidosis.
  • Electrocardiograph:
    • Findings: Atrial fibrillation, extrasystoles, AV block, other arrhythmias.
  • Chest X-ray:
    • Findings: Alveolar infiltrates, nodular densities, consolidation, which could represent alveolar haemorrhage, ARDS, pulmonary edema.
  • Lumbar Puncture:
    • Findings: Neutrophilic or lymphocytic pleocytosis, mild protein elevation, normal glucose.

Clinical Management

  • Empirical Antibiotics:
    • Mild Disease:
      • Preferred: Doxycycline (100 mg twice daily).
      • Alternatives: Amoxicillin, erythromycin.
    • Severe Infection:
      • IV Benzylpenicillin (1.2 g six-hourly) or ceftriaxone (1 g daily).
  • Jarish–Herxheimer Reaction:
    • Features: Sudden onset of shivers or rigors, fever, hypotension.
    • Cause: Acute inflammatory response from rapid death of Leptospira.
  • Life-threatening Complications:
    • Referral to hospital for further management.
    • Possible interventions: IV fluids, inotropes, ventilation, haemodialysis, treatment of arrhythmias and coagulopathies.
  • Corticosteroids:
    • Currently not recommended due to conflicting evidence and risk of nosocomial infections in severe cases.

Surveillance, Prevention, and Control of Leptospirosis

Surveillance:

  • Leptospirosis is a notifiable disease, mandatory reporting to NNDSS.
  • Public health units investigate cases, explore risk factors, and potential infection sources.

Infection Risk Reduction:

  • Avoid Direct Contact:
    • Contaminated soil or water, particularly floodwaters.
    • Animals or animal products.
  • Occupational Risk:
    • Target groups: farmers, abattoir and meat workers, banana workers, military personnel.
    • Educational materials about preventive measures.
    • Use of protective gear (boots, goggles, aprons, gloves).
    • Clean and cover open wounds.
    • Thorough washing after exposure.
  • Travelers:
    • Avoid floodwaters, swimming in rivers, and waterfalls after heavy rainfall in tropical developing countries.
    • Seek medical care promptly if a febrile illness develops.

Environmental Control Measures:

  • Livestock vaccination.
  • Segregating infected animals.
  • Rodent control.
  • Flood mitigation.
  • Reducing garbage to prevent rodent attraction and drain blockage.
  • Managing identified sources of infection from case investigations.
  • Issuing public health warnings and alerts during high-risk periods (e.g., post-flooding).

Prophylaxis:

  • Doxycycline:
    • Regular use (200 mg weekly) associated with nausea and vomiting, no clear benefit for reducing risk.
    • Not recommended routinely.
    • Considered for short-term intense exposures (e.g., soldiers, outbreak response personnel, recreational exposure) or after high-risk exposures (e.g., floodwaters).
    • Provides protection against other infectious diseases (e.g., malaria, rickettsia).
    • For travelers to malaria-endemic areas, consider doxycycline for malaria prophylaxis if at risk of leptospirosis.

Human Vaccines:

  • Rarely used due to limited effectiveness, adverse reactions, and short duration of protection.
  • No vaccines available in Australia.

You May Also Like

Leave a Reply

Your email address will not be published. Required fields are marked *

This site uses Akismet to reduce spam. Learn how your comment data is processed.