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Ebola Virus Disease.Care & specialists in Indonesia

In Indonesia, ebola Virus Disease is managed by tropical medicines. Ebola virus disease is a severe and often fatal filoviral illness transmitted through direct contact with the blood or other body fluids of infected people, primates, or fruit bats, with case-fatality rates of 25-90% across outbreaks and a median around 50%. The 2014-2016 West African outbreak — the largest in recorded history — caused 28,616 confirmed and probable cases and 11,310 deaths across Guinea, Liberia, and Sierra Leone; the 10th Democratic Republic of Congo outbreak in 2018-2020 caused 3,470 cases and 2,287 deaths; and the 2022 Sudan-strain outbreak in Uganda killed 55 of 142 confirmed cases.

aliases · Ebola virus disease (Ebola hemorrhagic fever)· Ebola hemorrhagic fever· Maladie à virus Ebola· Ugonjwa wa Ebola· reviewed May 14, 2026

Reviewed by AIHealz Medical Editorial Board · Tropical MedicineLast reviewed May 13, 2026

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§ 01

What it is

Ebola virus disease (ICD-10: A98.4) is a severe, often fatal viral hemorrhagic fever caused by infection with one of six recognized Ebola virus species in the family Filoviridae: Zaire ebolavirus (most virulent, responsible for the largest outbreaks and the target of approved vaccines and antibody treatments), Sudan ebolavirus (case-fatality 40-60% across outbreaks), Bundibugyo ebolavirus (case-fatality 25-40%), Taï Forest ebolavirus (a single recorded human case), Reston ebolavirus (asymptomatic in humans), and Bombali ebolavirus (recently identified, no confirmed human disease). Ebola virus is a single-stranded negative-sense RNA filovirus that infects monocytes, macrophages, and dendritic cells, then spreads systemically to liver, spleen, adrenal glands, and endothelium, causing massive cytokine release, coagulopathy, vascular leakage, and multi-organ failure. The natural reservoir is the African fruit bat (Pteropodidae family); primary human infection follows contact with infected bats or non-human primates, after which the virus spreads person-to-person through direct contact with blood, vomitus, stool, sweat, breast milk, semen, saliva, and contaminated surfaces. Outbreaks occur predominantly in equatorial sub-Saharan Africa, with sporadic cases imported by infected travellers.

key facts

Prevalence: Cumulative recorded cases since first identification in 1976 exceed 35,000, with more than 15,000 deaths across more than 30 outbreaks (WHO 2024)
Demographics: All ages affected; healthcare workers, family caregivers, and burial-rite participants carry the highest occupational risk
Avg. age: Median age at infection 25-35 years across major outbreaks
Global cases: More than 35,000 cumulative recorded cases since 1976; case-fatality rate 25-90% across outbreaks (median ~50%); Zaire ebolavirus strain has the highest CFR
Specialist: Tropical Medicine

§ 02

How you might notice it

01Sudden onset of fever above 38 °C, severe frontal headache, profound fatigue, and diffuse muscle and joint pain 2-21 days (average 8-10 days) after exposure.

02Sore throat with painful swallowing, chest pain, dry cough, and conjunctival injection in the first 3-5 days.

03Profuse watery diarrhoea, recurrent vomiting, severe epigastric and right-upper-quadrant abdominal pain, and progressive dehydration starting day 3-7.

04Maculopapular rash on the trunk, back, and limbs around day 5-7 — present in roughly 25-50% of patients and easily missed on dark skin.

§ 03

How it’s diagnosed

diagnosis

Clinical diagnosis is suspected in any patient with fever and compatible symptoms who has had potential exposure within 21 days (the maximum incubation period): travel from an active outbreak zone, contact with a known case, healthcare or laboratory work with Ebola samples, contact with bushmeat or wildlife, or unprotected sexual contact with a male survivor. Laboratory confirmation is by real-time reverse transcription polymerase chain reaction (RT-PCR) on blood, performed in a designated biosafety level 3 or 4 facility or with WHO-approved field cartridge platforms (such as GeneXpert). Detection of viral antigen by ELISA and IgM/IgG serology confirm exposure and recovery. Diagnostic yield rises after symptom day 3 — early in illness, viral load may be below detection thresholds and a negative test must be repeated 48-72 hours later if clinical suspicion remains high. Differential diagnosis is broad and includes other viral hemorrhagic fevers (Marburg, Lassa, Crimean-Congo, yellow fever), malaria (which must be ruled out and treated empirically while awaiting Ebola results), typhoid, shigellosis, leptospirosis, meningococcaemia, and severe sepsis from any cause. All suspected cases are isolated immediately in a designated Ebola treatment unit with strict PPE protocols. Imaging and ancillary investigations focus on assessing the severity of dehydration, organ injury, and coagulopathy: complete blood count typically shows leukopenia early, thrombocytopenia, and lymphopenia, with transaminitis (AST > ALT), elevated creatinine, and prolonged prothrombin time.

Key tests

Real-time RT-PCR for Ebola virus RNAConfirms acute Ebola virus infection — diagnostic standard during outbreaks

Antigen capture ELISADetects circulating Ebola antigen; useful when PCR not available and in field laboratories

IgM and IgG serology

§ 04

Treatment & cost

medical treatments

✓Inmazeb (atoltivimab/maftivimab/odesivimab, intravenous, single dose 50 mg/kg each component)
✓Ebanga (ansuvimab-zykl, intravenous, single dose 50 mg/kg)
✓Aggressive intravenous fluid and electrolyte resuscitation
✓Broad-spectrum empirical antibiotics

surgical options

Renal replacement therapy (continuous or intermittent hemodialysis)Improves survival in selected patients with isolated renal failure when delivered in advanced units; case-series mortality benefit roughly 20-30%

§ 05

Causes & risk factors

known causes

Zoonotic spillover from infected bats or non-human primates: Pteropodid fruit bats are the suspected natural reservoir. Index cases of outbreaks typically arise from handling, butchering, or eating infected bats, chimpanzees, gorillas, antelope, or duikers. Spillover events are rare but consistently the entry point of human outbreaks.
Direct human-to-human contact with infected body fluids: Once introduced into humans, Ebola spreads through direct contact with blood, vomitus, stool, saliva, sweat, breast milk, semen, urine, tears, and contaminated surfaces. Skin and mucous membranes are entry points; intact skin can also be sufficient for transmission. Highest risk during late disease and after death.
Healthcare exposures without adequate PPE: Healthcare workers and caregivers face elevated risk from needlesticks, splashes, and contact with patient fluids. In the 2014-2016 outbreak, over 800 healthcare workers were infected and over 500 died. Strict PPE protocols and dedicated Ebola treatment units have substantially reduced this risk.
Traditional burial practices: Direct contact with the body of a deceased person during washing, dressing, and traditional burial ceremonies has driven many transmission chains. Safe and dignified burial protocols designed in collaboration with communities are now standard outbreak response.
Sexual transmission and persistence in semen: Ebola virus persists in semen of male survivors for months — viable virus has been detected up to 9-12 months and viral RNA beyond 2 years. Documented sexual transmission has triggered new outbreak clusters, and WHO recommends abstinence or condom use until semen has tested negative twice.
Mother-to-child transmission: Pregnant women with Ebola infection have very high maternal and fetal mortality and the virus is transmitted through breast milk. Survivors who become pregnant or breastfeed can transmit the virus from persistently infected tissue.

§ 06

Living with it

01Receive rVSV-ZEBOV (Ervebo) ring vaccination if identified as a contact or contact-of-contact of a Zaire ebolavirus case.

02Pre-exposure vaccination with Ervebo or the two-dose Zabdeno/Mvabea regimen is offered to healthcare workers, laboratory staff, and outbreak responders in or travelling to active outbreak zones.

03Avoid contact with bats, non-human primates, and other potentially infected wildlife and do not consume bushmeat in endemic regions.

04Use full personal protective equipment when caring for any patient with suspected viral hemorrhagic fever, including impermeable gown, double gloves, N95 respirator or PAPR, and face shield.

05Practice safe and dignified burial — bodies of suspected or confirmed cases are handled only by trained teams using sealed body bags and protective equipment.

06Male survivors should use condoms or abstain from sex until two consecutive monthly semen RT-PCR tests are negative.

07Maintain regular handwashing with soap and water or 0.05% chlorine solution in healthcare and outbreak settings.

recommended foods

§ 07

When to seek help

why see a tropical medicine

Suspected Ebola requires immediate isolation in a designated treatment unit staffed by infectious disease, emergency, and critical care teams trained in biosafety protocols. Outside outbreak zones, suspected imported cases are coordinated by national public-health authorities, with reference laboratories handling all sample testing. Antibody treatment must be available within 24-48 hours of confirmation.

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01Hypovolemic and septic shock with multi-organ failure — leading cause of death; addressed with aggressive supportive care.

02Severe coagulopathy with disseminated intravascular coagulation and hemorrhage from multiple sites.

03Acute kidney injury requiring renal replacement therapy.

04Encephalopathy, seizures, and delayed neurological sequelae from direct CNS involvement.

05Persistent Ebola viral RNA in semen, eye, CNS, breast milk producing risk of late transmission and relapse.

06Uveitis and other ocular complications (in roughly 25-50% of survivors) that can lead to vision loss if untreated.

Related conditions

Marburg virus diseaseClosely related filovirus causing a clinically indistinguishable viral hemorrhagic fever; managed with the same isolation and supportive-care principles.Read →Lassa feverAnother West African viral hemorrhagic fever; differential diagnosis and outbreak response infrastructure overlap.Read →Yellow FeverVaccine-preventable hemorrhagic flavivirus also endemic in sub-Saharan Africa; differential for fever in returning travellers.Read →Dengue FeverGlobally common arboviral hemorrhagic illness; useful differential in returning travellers with fever and bleeding.Read →MalariaThe dominant febrile illness in sub-Saharan Africa and a frequent coinfection; always tested and treated empirically in suspected Ebola.Read →

Easily confused with

vs. Ebola Virus Disease

MalariaBoth present with high fever, headache, and myalgia in returning travellers from sub-Saharan Africa. Malaria is diagnosed by blood smear or rapid antigen test and responds to artemisinin therapy. Ebola is confirmed by RT-PCR and treated with monoclonal antibodies and intensive supportive care. Coinfection is common and malaria treatment is given empirically while awaiting Ebola results.Compare →

vs. Ebola Virus Disease

Marburg virus diseaseMarburg virus is a closely related filovirus that causes a clinically indistinguishable viral hemorrhagic fever. Discrimination requires RT-PCR. Marburg outbreaks have occurred in Angola, Uganda, Rwanda, Equatorial Guinea, and Tanzania. No licensed vaccine or antibody therapy exists for Marburg as of 2026.Compare →

vs. Ebola Virus Disease

Lassa feverLassa is an arenavirus transmitted predominantly by Mastomys rodents in West Africa. Onset is more gradual than Ebola, hearing loss is a hallmark complication, and ribavirin therapy reduces mortality. RT-PCR distinguishes the two.Compare →

vs. Ebola Virus Disease

Typhoid feverTyphoid produces a more gradual rising fever with abdominal pain, hepatosplenomegaly, and rose spots; bleeding is rare and confined to gastrointestinal hemorrhage from terminal-ileum ulcers. Diagnosed by blood culture; treated with ceftriaxone or fluoroquinolones.Compare →

Often appears alongside

Malaria →Typhoid fever →

Types and stages

Zaire ebolavirus (Ebola virus)First identified in 1976 in Yambuku, Zaire (now DRC). Most lethal species with case-fatality rates of 60-90% historically and 30-65% in recent outbreaks with modern care. Caused the 2014-2016 West Africa outbreak and the 2018-2020 DRC outbreak. Approved vaccine (Ervebo, rVSV-ZEBOV) and antibody treatments (Inmazeb, Ebanga) target this species.

Sudan ebolavirusFirst identified in 1976 in Sudan. Case-fatality 40-60% across outbreaks. Caused the 2000-2001 Uganda outbreak and the 2022 Uganda outbreak (142 cases, 55 deaths). No species-specific licensed vaccine or antibody, although candidate vaccines are advancing.

Bundibugyo ebolavirusIdentified in 2007 in western Uganda. Case-fatality 25-40%. Caused outbreaks in Uganda (2007, 2012) and DRC (2012). Closer antigenic relationship to Zaire and Sudan viruses than to Taï Forest.

Taï Forest ebolavirusSingle recorded human case in 1994 in a Swiss ethologist examining chimpanzees in Ivory Coast. Patient survived. No further human cases recorded.

Reston ebolavirusIdentified in 1989 in cynomolgus monkeys imported to Reston, Virginia. Causes lethal disease in non-human primates but has produced only asymptomatic seroconversion in humans. Circulates in pigs and primates in the Philippines.

Bombali ebolavirusIdentified in 2018 in insectivorous bats in Sierra Leone. No confirmed human cases; pathogenicity in humans unknown.

Living with Ebola Virus Disease

Timeline

Acute illness lasts 6-16 days; survivors typically improve from day 7-10 onwards. Most patients are discharged once two consecutive RT-PCR tests are negative on blood. Convalescence with fatigue, arthralgia, and weight loss lasts 1-3 months in mild cases and up to 12 months in severe cases. Post-Ebola syndrome symptoms (joint pain, eye disease, mental-health symptoms) follow a variable course and require structured 1-year follow-up. Semen RT-PCR is repeated monthly until negative twice consecutively, often 6-12 months and sometimes longer.

Lifestyle

01Survivors should attend structured one-year follow-up clinics for post-Ebola syndrome screening (joint pain, vision, neurological symptoms, mental health).
02Male survivors must use condoms or abstain from sex until semen testing confirms clearance (typically 6-12 months but occasionally longer).
03Healthcare workers in endemic regions should remain up to date with PPE training and vaccination.
04Travellers returning from outbreak zones should self-monitor temperature for 21 days and seek care immediately for fever.
05Community members should engage with public-health teams during outbreaks rather than hide cases, which prolongs transmission and outbreak duration.

Daily management

01Strict isolation and PPE protocols within the treatment unit until two consecutive negative RT-PCR tests confirm viral clearance.

Complementary approaches

Convalescent plasma from Ebola survivorsHistorical option used during early outbreaks and the 2014-2016 epidemic. Phase 2/3 trials (Ebola-Tx, van Griensven NEJM 2016) showed no clear survival benefit. Replaced by approved monoclonal antibodies.

Investigational antiviral therapy (remdesivir, favipiravir)Remdesivir and favipiravir were used in compassionate-access settings during the 2014-2016 and 2018-2020 outbreaks. Remdesivir was inferior to monoclonal antibodies in the PALM trial. Roles outside trials are limited.

Choosing a doctor

In an outbreak setting, care is delivered through designated Ebola treatment units coordinated by the ministry of health, WHO, MSF, and partners. In non-endemic regions, suspected cases are referred to a national high-consequence infectious disease unit (CDC-designated regional Ebola treatment centre in the US; high-consequence infectious diseases network in the UK). Patients should not be transported to non-designated facilities once Ebola is suspected.

Patient support resources

WHO Ebola virus disease — fact sheets and outbreak situation reports →Global epidemiology, outbreak history, current treatment and vaccine guidance, and live situation reports during outbreaks.

CDC Ebola (Ebola Virus Disease) →Clinical, laboratory, and public-health guidance for clinicians, travelers, and the public in the US and globally.

Médecins Sans Frontières (MSF) — Ebola response →Operational guidance, field reports, and survivor-care insights from MSF, the lead non-governmental responder in many outbreaks.

Africa CDC Emergency Operations Centre →African Union public-health body coordinating regional outbreak response and surveillance.

§ 08

Frequently asked

What is Ebola virus disease?

Ebola virus disease is a severe and often fatal viral hemorrhagic fever caused by Ebola viruses. It spreads through direct contact with body fluids of infected people or wildlife. Case-fatality rates have ranged from 25 to 90% across outbreaks, with a median around 50%. Approved vaccines and antibody treatments now cut mortality substantially for the Zaire strain.

How does Ebola spread?

Ebola spreads through direct contact with blood, vomit, stool, urine, sweat, breast milk, semen, and saliva of infected people, or contaminated surfaces. Sexual transmission from male survivors can occur for months. Bats are the suspected reservoir and primates can transmit to humans. It is not airborne.

What are the first symptoms of Ebola?

Early symptoms appear 2-21 days after exposure (average 8-10 days): sudden fever, severe headache, muscle and joint pain, profound fatigue, and sore throat. By day 3-7 vomiting, diarrhoea, abdominal pain, and a maculopapular rash appear. Hemorrhagic features develop in 30-50% of severe cases.

How long does Ebola incubation last?

The incubation period is 2 to 21 days, with most cases developing symptoms 8-10 days after exposure. Anyone exposed who remains symptom-free for 21 days is not infected. People are not infectious during incubation; transmission requires symptoms.

Is there a cure for Ebola?

Two approved monoclonal antibody treatments — Inmazeb (atoltivimab/maftivimab/odesivimab) and Ebanga (ansuvimab) — reduce mortality of Zaire ebolavirus infection from over 50% to under 35% when given early. They are not yet effective against Sudan or Bundibugyo strains. Aggressive supportive care remains the foundation of treatment.

Is there an Ebola vaccine?

Yes. The rVSV-ZEBOV vaccine (Ervebo) is over 97% effective against Zaire ebolavirus and was licensed in the US and EU in 2019. A two-dose Zabdeno/Mvabea regimen offers durable protection. No species-specific licensed vaccine exists for Sudan or Bundibugyo as of 2026, although candidate vaccines are in trials.

Can you survive Ebola?

Yes. Survival has improved dramatically with modern care. Patients treated early with monoclonal antibodies and aggressive supportive care have mortality of 25-35% for Zaire ebolavirus and under 20% if the viral load is low at treatment start. Tens of thousands of people have survived Ebola.

What is post-Ebola syndrome?

Post-Ebola syndrome refers to long-term sequelae in survivors: arthralgia in about 75%, uveitis or other ocular symptoms in 25-50%, fatigue, headache, hearing changes, neurological complications, depression, and anxiety. Most symptoms improve over 1-2 years; some are permanent. Structured 1-year follow-up is standard.

How is Ebola diagnosed?

Diagnosis is confirmed by real-time RT-PCR for Ebola viral RNA on blood, performed in a designated biosafety laboratory or with field cartridge platforms (such as GeneXpert Ebola). Antigen ELISA and IgM serology support diagnosis. Sensitivity improves after symptom day 3, and negative tests are repeated in 48-72 hours if suspicion remains high.

Where are Ebola outbreaks happening?

Ebola outbreaks occur predominantly in equatorial sub-Saharan Africa. The largest recorded outbreak (2014-2016) struck Guinea, Liberia, and Sierra Leone. Major outbreaks have also occurred in DRC, Uganda, Sudan, Republic of Congo, Gabon, Côte d'Ivoire, Mali, and Nigeria. The 2022 Uganda outbreak involved the Sudan strain.

Can Ebola survivors transmit the virus?

Yes, in specific circumstances. Ebola virus persists in semen, ocular fluid, breast milk, and central nervous system of survivors for months. Sexual transmission and breast-milk transmission have triggered new outbreaks. WHO advises condom use until two consecutive monthly semen RT-PCR tests are negative.

How is Ebola spread different from COVID-19?

COVID-19 spreads through respiratory droplets and aerosols and is highly transmissible. Ebola requires direct contact with body fluids of a symptomatic patient or recently deceased person and is not airborne. This is why Ebola outbreaks are typically smaller and more geographically limited than respiratory viral outbreaks.

What does Ebola treatment involve?

Treatment combines monoclonal antibodies for Zaire ebolavirus (Inmazeb or Ebanga), aggressive intravenous fluid and electrolyte resuscitation, empirical antibiotics and antimalarials, symptomatic care (antiemetics, analgesia, oxygen), and organ support including renal replacement when needed. Care is delivered in designated treatment units with full personal protective equipment.

Is Ebola airborne?

No. Ebola is not transmitted through casual airborne spread under normal patient-care conditions. Aerosolization can occur during certain medical procedures (such as suctioning), and these are managed with airborne-precaution PPE. Outside hospital settings, transmission requires direct contact with body fluids.

What is ring vaccination?

Ring vaccination is rapid vaccination of all contacts and contacts-of-contacts of a confirmed Ebola case, plus frontline workers, to surround new infections with immune individuals. It uses the rVSV-ZEBOV vaccine and has been the cornerstone of containment since 2015. Ring vaccination has contributed to dramatic shortening of outbreaks.

Can children get Ebola?

Yes. Children account for roughly 20% of cases in major outbreaks. Outcomes are worst in infants and neonates; older children and adolescents have outcomes similar to young adults. Pediatric care follows the same principles as adult care with weight-based fluid and drug dosing.

Is Ebola contagious before symptoms appear?

No. People do not transmit Ebola during incubation; transmission requires symptoms and the presence of detectable virus in body fluids. Contacts who remain symptom-free for 21 days after exposure are not infected. Contact tracing is built around this 21-day window.

Can Ebola virus disease come back?

Late recrudescence has been documented in survivors with persistent virus in immune-privileged sites (eye, central nervous system, semen) and in survivors who develop new symptomatic disease months to years later. The 2021 Guinea outbreak was traced genetically to a survivor of the 2014-2016 epidemic, indicating very long-term viral persistence.

Is Ebola treatment available outside Africa?

Yes. Suspected cases in non-endemic regions are referred to designated high-consequence infectious disease units (such as CDC-designated regional Ebola treatment centres in the US). Monoclonal antibody therapy and rVSV-ZEBOV vaccine are available through national stockpiles, the WHO emergency reserve, and the International Coordinating Group on Vaccine Provision.

What PPE is needed for Ebola care?

Healthcare workers in Ebola treatment units wear impermeable gown, double gloves, N95 or PAPR respirator, full face shield, head cover, and waterproof boots. Donning and doffing are performed under supervision to prevent self-contamination. Adherence to PPE protocols cut healthcare-worker mortality dramatically after the 2014-2016 outbreak.

How are Ebola outbreaks contained?

Outbreak containment combines rapid case identification through RT-PCR, contact tracing of all known exposures, ring vaccination with rVSV-ZEBOV, dedicated treatment units, safe and dignified burial, community engagement and trust-building, infection prevention and control in healthcare, and laboratory surveillance. Most outbreaks are contained within 6-22 months under modern response.

§ 09

Sources & references

01
World Health Organization. Ebola virus disease fact sheet. WHO Geneva, 2024.accessed 2026-05-14
02
Mulangu S, Dodd LE, Davey RT Jr, et al. 2019. A randomized, controlled trial of Ebola virus disease therapeutics (PALM trial). New England Journal of Medicine 381(24):2293-2303.accessed 2026-05-14
03
Henao-Restrepo AM, Camacho A, Longini IM, et al. 2017. Efficacy and effectiveness of an rVSV-vectored vaccine in preventing Ebola virus disease (Ebola Ça Suffit ring vaccination). Lancet 389(10068):505-518.accessed 2026-05-14
04
Feldmann H, Geisbert TW. 2011. Ebola haemorrhagic fever. Lancet 377(9768):849-62.accessed 2026-05-14
05
Jacob ST, Crozier I, Fischer WA II, et al. 2020. Ebola virus disease. Nature Reviews Disease Primers 6(1):13.accessed 2026-05-14
06

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