In Indonesia, melioidosis is managed by infectious diseases. Melioidosis is a tropical bacterial infection caused by Burkholderia pseudomallei, an environmental saprophyte found in soil and surface water across northern Australia, Southeast Asia, the Indian subcontinent, and increasingly recognized in Africa and the Americas. A 2016 modeling study estimated 165,000 human cases per year worldwide with 89,000 deaths, making it one of the most underdiagnosed killers in the tropics.

Melioidosis (ICD-10: A24) is an infectious disease caused by Burkholderia pseudomallei, a Gram-negative bacillus that lives freely in soil and water across tropical and subtropical regions. The organism enters humans through skin inoculation, inhalation of aerosolized soil or water, or ingestion of contaminated water; person-to-person transmission is extremely rare. Once inside the host, B. pseudomallei is a facultative intracellular pathogen that can survive within macrophages and persist as a latent infection for years to decades before reactivation.
The key symptoms of Melioidosis are: Fever above 38°C with rigors, present in over 90% of acute cases and often the first sign., Cough with purulent or blood-streaked sputum, present in roughly half of patients and reflecting pulmonary involvement., Pleuritic chest pain with shortness of breath when consolidation or pleural effusion is established., Skin ulcer, abscess, or non-healing wound at a site of soil or water contact — often the only initial sign in localized disease., Joint pain and swelling, particularly in large weight-bearing joints (knee, hip), suggesting septic arthritis., Urinary frequency, dysuria, perineal pain, or acute urinary retention in prostatic abscess — a male-predominant complication., Right upper quadrant or left upper quadrant abdominal pain suggesting hepatic or splenic abscesses..

Diagnosis of melioidosis depends on awareness, microbiological isolation, and supportive imaging. In endemic regions, any patient with sepsis, pneumonia, or visceral abscess — especially with diabetes — should be tested for B. pseudomallei. Outside endemic areas, travel history is critical: melioidosis must be considered in returning travelers from northern Australia, Southeast Asia, the Indian subcontinent, and increasingly Africa and the Americas. The diagnostic gold standard is culture of B. pseudomallei from blood, sputum, urine, pus, or other normally sterile site using Ashdown's selective medium. The organism grows in 24-72 hours but can be initially misidentified by automated systems as Pseudomonas or another organism — laboratories in endemic regions are trained to recognize the characteristic wrinkled colony morphology and bipolar safety-pin Gram-stain appearance. The 2020 international consensus guidelines recommend immediate isolation precautions (BSL-3 in non-endemic regions) once melioidosis is suspected, due to laboratory-acquired infection risk. Imaging with chest X-ray and CT of the chest and abdomen identifies pulmonary consolidation, splenic and hepatic abscesses, and prostatic involvement. Splenic micro-abscesses on CT in an endemic-region patient with fever should suggest melioidosis until proven otherwise. Serologic tests including indirect hemagglutination assay support diagnosis in chronic or culture-negative cases but lack the specificity needed for acute diagnosis in endemic populations. Newer rapid lateral-flow antigen tests (Active Melioidosis Detect) are emerging for resource-limited settings.
Mortality from melioidosis depends on geography, presentation, and access to care. In northern Australia with intensive care and protocolized therapy, acute mortality has fallen from 30% in the 1990s to approximately 10% today (Currie 2021 Darwin Prospective). In northeast Thailand, where many patients present late and access to ICU is limited, acute mortality remains 30-40%. Septic shock at presentation carries a mortality of 50% or more even with treatment. Neurological melioidosis has substantial residual deficits in survivors. Relapse occurs in 5-15% within 1-2 years of completing therapy when the full 3-6 month eradication phase is taken, and exceeds 25% when eradication therapy is shortened or omitted. Diabetes, alcohol use, and renal disease independently predict worse outcomes. Long-term survivors who complete therapy and control underlying conditions can expect a return to baseline health, though latent reactivation decades later is well-documented.
Melioidosis is a life-threatening infection that should be managed by an infectious disease specialist with hospital experience. In endemic regions, presumptive treatment with ceftazidime or meropenem is often started in emergency departments while awaiting culture confirmation. In non-endemic regions, an infectious disease consultation is essential because most clinicians have no direct experience and the organism is intrinsically resistant to many empirical antibiotic regimens.
Find specialists →Symptom improvement typically begins within 3-7 days of starting effective intravenous therapy; persistent fever after 10-14 days suggests inadequate source control or deep undrained collection. The intensive intravenous phase lasts 10-14 days for uncomplicated disease and 4-8 weeks for complicated disease. The oral eradication phase runs 3 months for skin or pulmonary disease and 6 months for deep-seated, neurological, bone, or joint involvement. Surveillance for relapse continues to 12 months after the end of therapy.
During acute infection and the intensive antibiotic phase, rest and gradual mobilization as tolerated are appropriate. After hospital discharge and once the eradication phase is established, light to moderate exercise can resume as energy permits — typically over 4-12 weeks. Avoid renewed soil or water exposure in endemic regions until the full course is complete.
Look for an infectious disease physician with tropical medicine training or experience in endemic regions. Care should be delivered in a hospital with intensive care, microbiology capable of identifying B. pseudomallei, and interventional radiology for abscess drainage. In non-endemic regions, telemedicine consultation with reference centers (Royal Darwin Hospital, Mahidol-Oxford Tropical Medicine Research Unit, CDC) is appropriate.
Medically reviewed by AIHealz Medical Editorial Board · May 13, 2026
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