Ebola Virus Disease

Caitlyn Hollingshead; Helena Swinkels; Sumir Shah

Ebola Virus Disease

Earn CME/CE in your profession:

Free Review Questions

Continuing Education Activity

Ebola viruses are contagious, lethal viruses that are the causative agents of rare Ebola virus disease. Ebola virus disease presents with nonspecific symptoms, including fever, malaise, headache, diarrhea, and vomiting. A maculopapular rash is sometimes noted. Bleeding, often manifesting as oozing from venipuncture sites, hematochezia or melena, hematemesis, or bleeding from the gums, occurs in less than 50% of cases. Highly transmissible, it can cause large outbreaks, epidemics, and pandemics. Despite outbreak control efforts, the Western African epidemic from 2013 to 2016 affected several countries outside continental Africa. An epidemic can have a devastating global impact on healthcare, economy, and society. Treatment is mainly supportive; investigational therapies continue to be researched. This activity describes the evaluation, treatment, and management of patients infected with Ebolavirus and explains the role of the healthcare team in limiting the spread of the virus.

Objectives:

Identify the etiology and pathogenesis of Ebola-related medical conditions and emergencies.
Identify risk factors for Ebola virus disease.
Select appropriate therapies for patients with Ebola virus disease.
Collaborate with other healthcare professionals to institute effective infection and other communicable disease control procedures to safely provide patient care for patients with or under investigation for Ebola virus disease and to limit its spread in the community.

Introduction

Ebola viruses are contagious, lethal viruses that are the causative agents of rare Ebola virus disease. Ebola virus disease, once known as Ebola hemorrhagic fever, can cause oozing from venipuncture sites, melena, hematochezia, and hematemesis. However, these manifestations are seen less than 50% of the time.[1] Nonspecific symptoms, including fever, malaise, headache, and myalgias, are common initial symptoms.[2] Diarrhea, nausea, and vomiting begin a few days later and can be severe.

The disease can quickly progress to multiorgan system failure, leading to shock and death. The overall case-fatality rate is about 40% to 50%.[3] The main variables impacting survival rate are early disease identification and access to healthcare for patient stabilization and supportive medical care, differences in health status (such as nutrition and coinfections), genetic differences, and patient attitudes surrounding seeking medical treatment.[3]

Highly transmissible, it can cause large outbreaks, epidemics, and pandemics. Despite outbreak control efforts, the Western African epidemic from 2013 to 2016 affected several countries outside continental Africa. An epidemic can have a devastating global impact on healthcare, the economy, and society. Treatment is mainly supportive; investigational therapies continue to be researched.

Ebola viruses, filamentous viruses with a characteristic twisted thread shape belonging to the Filoviridae family, were discovered in The Democratic Republic of Congo in 1976.[3][4] Filoviridae are negative-strand RNA viruses and derive their name from the Latin word "filum," meaning thread.[4] This viral family most commonly infects humans and primates and is thought to use fruit bats of the Pteropodidae family as a natural reservoir.[5][6]

Due to the high transmissibility and lethality of Ebola viruses, high clinical suspicion and early diagnosis are vital to reduce mortality and the risk of an Ebola outbreak. Improved diagnostics, therapeutics, and vaccines have become available in the last few years, improving survival and decreasing the potential for spread. Adequate Infection Prevention and Control (IPC) measures must be implemented rapidly to prevent spread in healthcare facilities. Urgent reporting to Public Health allows contact tracing, surveillance, and other public health measures to be promptly implemented in the community.

To reduce the risks of Ebola epidemics and the potential misuse of the virus as an agent of bioterrorism, research is ongoing to further develop diagnostic tests, therapeutics, and vaccines.[1]

Etiology

Ebola viruses, named after the Ebola River, emerged in 1976. The viruses appear episodically in animal populations in regions close to the African equator. They are highly transmissible between humans and primates, including chimpanzees, apes, and gorillas.[7] Ebolavirus and Ebola virus antibodies can also be found in bats, which are considered asymptomatic reservoirs.[7][6] Although bats with Ebola virus antibodies have been discovered in surveillance studies during outbreaks, establishing a causal relationship with human illness remains unproven.[8]

Filoviridae family members to Ebolavirus are the Marburgvirus, extremely virulent in humans, and the Cuevavirus, which thus far has only been found in bats in Spain and Hungary.[9][1] The 5 subtypes of Ebola virus that cause clinical disease in humans are named based on topographic discovery: Zaire/Ebola (EBOV), Bundibugyo (BDBV), Sudan (SUDV), and more recently, Tai Forest (TAFV), and Bombali (BOMV).[10][7] No appreciable difference in virulence is observed across outbreaks induced by different subtypes.[3] Other filoviruses have been identified, but to date, these do not infect humans or do not cause clinical illness in humans.

The renaming of Ebola virus terms over time has complicated the filovirus taxonomy. Since 2018, Ebola virus, Ebola virus disease (EVD), and EBOV have explicitly referred to the Zaire subtype of Ebola viruses.[1] Ebola virus (species Zaire ebolavirus) has caused most Ebola virus outbreaks and is thus the most studied of the Ebolavirus types.

Electron microscopy of blood samples demonstrates the Ebola virus structure. The EBOV virion is surrounded by an envelope with glycoprotein (GP_1,2) spikes.[3] The single-stranded, negative-sense RNA core is packaged in the virion capsule with 4 proteins: NP, VP35, VP30, and L. These proteins and glycoproteins are important components of Ebola pathophysiology and immunogenicity.

Epidemiology

Since its discovery, over 25 EVD outbreaks have occurred; many were confined to rural areas in Sudan, the Democratic Republic of Congo, Gabon, the Republic of the Congo, and Uganda.[11] Ebola virus disease has claimed the lives of over 15,000 people.[12] Hunting and eating bushmeat is a risk for contracting Ebola viruses.[13] Transmission in the community from the patient to family and community members and during funeral practices can be rapid.[14]

The most recent outbreak of Ebola virus disease occurred from April to September 2022 in the Democratic Republic of the Congo.[15] The largest and longest epidemic (late 2013 to 2016) spanned Western Africa, with cases also found in parts of Europe and the United States. Healthcare systems in some countries were overwhelmed, shedding light on the lack of preparedness for epidemics. Most reported cases outside of Africa were healthcare workers providing aid in regions with an active outbreak, who had strict travel restrictions and effective quarantine strategies; only a few travelers were infected due to direct human contact.

The case fatality rate of Ebola virus disease without supportive care or other treatments may be as high as 90%.[7] With heightened awareness, increased education on the importance of seeking medical care, and early detection, the average mortality rate has now reduced to approximately 50%. Persons are only infectious when experiencing symptoms of the infection, such as fever, chills, nausea, or vomiting, or when people come in contact with contaminated objects or infected deceased persons.[3] Due to its high case-fatality rate, the virus is a feared biowarfare agent.[16]

Transmission

Infected humans and non-human primates transmit Ebola viruses through direct contact with bodily fluids, including saliva, blood, urine, feces, sweat, breast milk, or semen, and contact with objects (or fomites).[1][7] The virus usually enters the new host through mucosal membranes and perhaps skin. It can occasionally happen percutaneously. Ebola viruses can persist in body fluids for prolonged periods. For example, in semen, Ebola virus has been isolated for up to 82 days [17] and detected via PCR up to 101 days after initial symptoms.[18] Cases of sexual transmission of Ebola viruses from semen and from pregnant mothers to their fetuses have occurred.[18][32080199]

Once it has entered the host, the virus incubates for an asymptomatic, noncontagious period, usually lasting several days to a few weeks. Patients are contagious once they start exhibiting signs and symptoms. The amount of time a virus can survive outside the human body is unknown. Most often, the bedding, clothes, and medical utensils utilized by patients are all burned or disposed of as medical waste to avoid contamination and the risk of spreading the virus.[19] Some traditional funerals in affected countries include opportunities to touch the bodies and personal items of persons who have died, which can contribute to the spread of the disease.[20]

Pathophysiology

Once the Ebola virus infects the host, there is an incubation period of 2 to 21 days, with a mean of 8 to 10 days.[7] The virus penetrates the host cell membrane by binding with GP_1,2, which triggers endocytosis. Once inside the cell, the virus releases its nucleocapsid into the host cell cytoplasm. VP30 initiates viral RNA replication [32080199] and serves as a regulatory protein; phosphorylation of VP30 by transcribed viral proteins turns off VP30 and ceases viral protein synthesis. Due to this unique function, VP30 has been identified as a target for vaccine development. The matrix protein VP40 is also produced and packaged into exosomes and is involved in host immune system suppression. Virus release from the cell is by budding from the cell membrane; this can cause direct damage to the cell and cell death. EBOV-specific cellular and humoral immune responses develop but are often outpaced by virus-host cell interactions. The process is not fully understood and continues to be investigated.

Mononuclear cells are among the cells that are first targeted by the virus.[7] The destruction of these cells results in the release of cytokines and reactive oxygen species responsible for edema and hypovolemic shock.[7] Destruction of other tissue cells results in myalgias from myositis, hepatitis, and acute kidney injury from renal tubular dysfunction.[1] Immune-mediated cell damage causes further injury, leading to dysfunction in multiple vital organs such as the lungs, heart, kidney, and liver.[21] The combined effects lead to multi-system organ failure. Death can occur quickly from the onset of symptoms, often within 6 days.[14] For survivors, long-term consequences have been identified, including hepatitis, encephalitis, uveitis, and spinal cord injury.[7]

Hemorrhagic responses are complex and involve disruption of the coagulation cascade through platelet aggregation, which sequesters platelets, causing bleeding and clotting simultaneously.[22] Liver damage also reduces the production of clotting factors.[22]

History and Physical

Persons infected with an Ebola virus present with sudden fever, malaise, headache, anorexia, and myalgias.[23] This is often followed by nausea, abdominal pain, vomiting, and diarrhea.[1][23] Red eyes, sore throat, and hiccups may also occur.[32080199] A maculopapular rash and hemorrhagic features such as bleeding from mucosal membranes, skin, eyes, nose, and ears may appear later in this early phase.[1][32080199] Shortness of breath and cough commonly occur as the syndrome progresses, as do neurologic symptoms, including confusion and prostration.[32080199][23][1]

The primary and most crucial evaluation is serial patient assessments with careful attention to vital signs and volume status.[1] Patients should be assessed for signs of dehydration, including mucous membranes and skin turgor. Fluid losses are often severe, averaging between 3 and 5 liters daily, but up to 10 liters/day.[24] On physical exam, a patient presenting early in illness may be noted to be relatively stable with prodromal symptoms. In contrast, patients later in infection, with higher viral loads, may be severely ill and in shock.

Most people with these symptoms do not have Ebola virus disease. However, clinical suspicion should be high in epizootic areas worldwide if the World Health Organization has declared an outbreak of international concern.

History includes:

Travel to an area with an Ebola outbreak within 2 to 21 days of symptom onset.
Contact with an ill person with suspected or confirmed Ebola or any contact with any object that might have come in contact with body fluids within the last 21 days.
Contact with semen from an Ebola Disease survivor
Any breach in Infection Prevention and Control procedures if caring for a suspected or confirmed Ebola case
Participation in certain activities while in an active outbreak region:
- Attending a funeral or preparing a body for funeral or burial
- Working or visiting a health facility or laboratory
- Visiting a traditional healer
- Contact with bats or animals
- Working or visiting a mine or cave.

If risk factors exist in the context of consistent signs and symptoms, the patient should be immediately isolated in a single room with a private bathroom or bedside commode, and Hospital Infection Prevention and Control should be contacted.

A careful history of sick and close contacts must be obtained for follow-up by local or state health authorities. Any suspected or confirmed cases of Ebola must be reported to the local or state health department as soon as possible, considering the need to stabilize and treat the patient.

Evaluation

Laboratory Testing

Laboratory tests to consider in patients diagnosed with Ebola virus disease or a person under investigation (PUI) for Ebola virus disease are:

Complete blood count testing is essential for evaluating hemoglobin, platelet, and leukocyte counts. Bleeding due to coagulopathy can result in severe anemia, resulting in the need for transfusion. Bacterial co-infections are also often present.[7]
A comprehensive metabolic panel helps evaluate acute kidney injury, electrolyte abnormalities (such as hyponatremia, hyperkalemia, and hypokalemia), elevated liver enzymes, and hypoglycemia that is often present.[25]
An arterial blood gas should be drawn to evaluate for acid-base disturbances.[25]
Creatine kinase testing should be sent to evaluate for rhabdomyolysis.[7]
A urinalysis should be done to assess for renal dysfunction.[7]
A basic coagulation profile, including prothrombin time, active partial thromboplastin time, fibrinogen, and international normalized ratio (INR), should be drawn and monitored to evaluate for signs of coagulopathy.[7]
A blood type and screen should be tested preemptively; a blood transfusion may be necessary to support the patient.[7]
A diagnostic test to evaluate for the presence of Ebola virus.[7]

Diagnostic Testing

Several molecular testing methods are available. RT-PCRs evaluate for the presence of the nucleoprotein or envelope glycoprotein.[26] These tests require an inactivation phase and must be performed in biosafety level 4 isolation.[26] Some reagents need to be kept at -20°C.[26] Additionally, the test requires a dedicated area and careful attention, as some byproducts of testing can contaminate the test. Testing generally requires 3 to 4 hours to perform. Although RT-PCRs are the most sensitive tests, the limitations of the safety requirements and equipment needed make this problematic in resource-limited settings. They are instead often found in reference laboratories. Automated nucleic acid tests are easier and quicker to perform. A comparative study comparing the RT-PCR method and an automated nucleic acid test, the FilmArray test, showed 85% agreement between the 2 tests.[27]

Several rapid lateral flow assays with quicker turnaround times than PCR testing are also available. A meta-analysis that compared rapid tests to RT-PCR showed a pooled sensitivity of 85% and a pooled specificity of 95%.[28] Some rapid tests have a sensitivity as low as 77%.[29] Although more sensitive and specific tests are needed, these remain potent tools in rural areas with limited resources and an epidemic setting.

Serologic tests can be helpful. However, the earliest that Ebola IgM can be detected is 6 days after the onset of the illness.[30] Due to the nature of Ebola virus disease, patients may have died before IgM would be detectable.

Radiography

Chest x-rays should be done to evaluate for pulmonary edema secondary to capillary leak syndrome.[31]

Treatment / Management

Infection Prevention and Control

The importance of employing immediate, effective Infection Prevention and Control (IPC) for patients with Ebola virus disease cannot be understated. The reproduction number of EBOV is estimated to be between 1.51 and 2.53, meaning for every patient infected with EBOV, between 1 and 3 additional people are expected to be infected.[32] Effective IPC is paramount to controlling the spread of EVD. In endemic areas in West Africa, patients are often directed to Ebola Treatment Units (ETUs) that have tight protocols for testing and isolation.[33] However, patients may first seek treatment at any healthcare facility or not at all. This is sometimes due to the belief that the ETUs were the source of the infection.[34] In areas with inadequate contact tracing, people infected with an Ebola virus may present to facilities that do not have adequate IPC measures. This can amplify spread, as happened in the West African EVD epidemic between late 2013 and 2016.[33] In this epidemic, more than 800 healthcare workers died of EVD; most of these occurred where adequate IPC precautions were not employed.[25]The ability to screen patients for symptoms and signs consistent with EVD, practical training on IPC, facilities to isolate patients with EVD and those under investigation, and swift reporting of patients suspected of having Ebola to public health agencies are crucial to an effective IPC effort to control the disease.[33]

The first case seen in the United States was in a community hospital in Dallas, Texas, in 2014.[35] Two nurses were infected while caring for the patient.[35] Following this, extra engineering controls were added for the medical intensive care unit to contain the virus, including zippered fabric walls to denote where PPE was required and the implementation of unidirectional entry and exit from the unit to decrease contamination of PPE.[35] Strict PPE was also implemented for laboratory personnel testing materials from patients with EVD or those under investigation.[35]

A Cochrane review found evidence about optimal PPE to be uncertain, with tradeoffs between effectiveness, comfort, and errors in donning and doffing.[36] Modifying PPE design may be effective. Spoken instructions during doffing, double gloving, glove disinfection, and following CDC guidance may improve effectiveness and compliance. The Centers for Disease Control and Prevention recommend:

single-use, impermeable gowns or coveralls
either a powered, air-purifying respirator (PAPR) or an N95 respirator with a hood from head to shoulders and a disposable face shield (in case an aerosol-generating procedure needs to be performed emergently)
two pairs of single-use gloves with extended cuffs
single-use boot covers
a single-use apron

PPE donning should occur with a trained observer who utilizes a written checklist and can ensure that PPE is worn correctly. PPE should be doffed in a designated area and placed in an infectious waste container. PPE should be inspected for any defects during the doffing process. Consistent and correct use of PPE and rapid initiation of isolation precautions effectively stop the chain of transmission; unfortunately, access to PPE has historically not been available in some areas affected by Ebola virus disease.[37]

The virus particle is resilient to inactivation. The virus is sensitive to sodium hypochlorite, gamma irradiation, high-dose ultraviolet light, and heat treatment (60 minutes at 60 °C or boiling for 5 minutes).[7]

Public Health Follow-up

Both suspected and confirmed cases of Ebola virus disease are reported to local or state health officials as appropriate to the location. A suspect case is one in which a patient's signs, symptoms, and risk factors are consistent with Ebola virus disease but without confirmatory testing.[CDC. Ebola Disease] A confirmed case is one in which laboratory confirmation has been made. Close contacts include anyone in direct contact with a person confirmed or suspected to be sick with Ebola or objects that may be contaminated with their bodily fluids.

Health officials will individually follow all close contacts for 21 days. They will also report the case to the CDC, as Ebola is internationally reportable under international health regulations.

International travel bans and exit screenings upon departure from countries with active Ebola outbreaks have previously been implemented to prevent further spread.[38] However, this may limit the ability of aid workers to reach affected countries and promote more circuitous routes into and out of affected areas, which may decrease the effectiveness of infection prevention efforts.[39]

Supportive Care

The cornerstone of management and treatment for patients infected with an Ebola virus and exhibiting symptoms of Ebola virus disease is supportive care. Oral rehydration is highly recommended for all patients able to drink.[25] Parenteral fluid replacement is recommended in patients unable to take an adequate amount of fluids via the oral route or for those patients whose ongoing fluid losses are greater than their oral intake.[25] Vital signs and careful assessment of fluid status should be done at regular intervals to assess whether fluids should be adjusted.[25] Assessing electrolytes and renal function is recommended as electrolyte abnormalities, such as hypokalemia, hyperkalemia, and hyponatremia, are independent predictors of mortality in patients with Ebola virus disease.[40][25] Adequate staffing ratios to enable quick recognition of status changes, communicating with family and friends to decrease psychological distress, and adequate analgesics to relieve pain are also recommended.[25] Additionally, broad-spectrum antibiotics should be administered to patients with severe illness as bacterial co-infections are often present.[25]

Therapeutics

The Pamoja Tulinde Maisha (PALM) trial solidified ansuvirimab and REGN-EB3 as preferred treatments for EVD over ZMapp and remdesivir.[31774950] Further information on this trial is below under "Pertinent Studies and Ongoing Trials." Ansuvirmab (MAb114) is an IgG1 monoclonal antibody that binds to the Ebola virus receptor binding domain.[41] It was approved by the US Food and Drug Administration (FDA) for Ebola treatment in December 2020.[42] REGN-EB3 combines 3 monoclonal antibodies that target Ebola virus glycoproteins: atolivimab, maftivimab, and odesivimab.[43] This drug obtained FDA approval in the United States in October 2020.[43]

Vaccinations

The live vesicular stomatitis virus-vectored vaccine against EBOV (r-VSV-ZEBOV) encodes a glycoprotein against EBOV.[44] Partial and maximal protection against death due to EBOV is achieved within 3 and 7 days, respectively, after one dose of vaccine in non-human primates.[44] The single-dose regimen makes it ideal for outbreak control for EBOV, using ring vaccination of primary and secondary contacts. It has been used effectively as post-exposure prophylaxis when more recent antibody therapies were unavailable.[44] In large human clinical trials, vaccine efficacy is 97.5% to 100% when given pre-exposure.[44] In a randomized clinical trial, 76% of adults and 87% of children receiving r-VSV-ZEBOV pre-exposure continued to have a detectable antibody response at twelve months.[45] The vaccination received US FDA approval for use in patients older than twelve months in August 2023.

Ad26.ZEBOV encodes a viral glycoprotein and utilizes an adenovirus 26 vector.[7] This is usually followed by a dose of MVA-BN-FILO, which encodes Ebola, Marburg, Sudan, and Tai Forest viruses using a modified vaccinia vector.[45][7] Forty-one percent of patients who received the Ad26.ZEBOV vaccination followed by the MVA-BN-FILO 56 days later had an antibody response twelve months post-vaccination.[45]

Differential Diagnosis

Ebola virus disease should be differentiated from other causes of hemorrhage in the febrile patient and common viral illnesses presenting with similar prodromes and gastrointestinal symptoms.

Hemorrhage in the Febrile Patient

Marburg virus
Crimean-congo hemorrhagic fever
Lassa fever
Rift Valley fever
Dengue
Bunyavirus

Similar Prodromal Symptoms

Malaria
Typhoid fever
Measles
Leptospirosis
Influenza
COVID-19 infection

Gastroenteritis

Shigella
Rotavirus
Norovirus

Pertinent Studies and Ongoing Trials

The Partnership for Research on EBOV in Liberia II (Prevail II) study was a randomized controlled trial performed in 2015 that randomized 72 patients to receive either ZMapp or only supportive care.[46] 37% of patients randomized to the supportive care arm died, compared to 22% in the ZMapp arm.[46] This study established that ZMapp was likely beneficial over only supportive care.

The Pamoja Tulinde Maisha (PALM) study was a randomized, controlled study performed in 2019 that evaluated EBOV patients receiving one of 4 agents:[47]

Ansuvirmab (MAb114) is an IgG1 monoclonal antibody that binds to the Ebola virus receptor binding domain.[41]
REGN-EB3 combines 3 monoclonal antibodies: atolivimab, maftivimab, and odesivimab.[43] These monoclonal antibodies target Ebola virus glycoproteins.[43]
Remdesivir is a pro-drug of a nucleoside analog that terminates RNA synthesis by inhibiting RNA-dependent RNA polymerase.[48] This pro-drug was initially developed to treat hepatitis C but was found to have wide-spectrum activity against RNA viruses.[49] This treatment was found to have activity in Ebola virus-infected primates.[49]
ZMapp is a mixture of monoclonal antibodies optimized from other monoclonal antibody cocktails. It showed early promise in the Partnership for Research on Infectious Diseases and Vaccines in Liberia (PREVAIL) II trial.[50][46]

In this trial, 673 people were randomized and included in the final analysis to receive one of the 4 treatments in equal ratios.[47] Based on the preliminary results of the trial revealing significantly lower mortality in the REGN-EB3 and Mab114 groups, further participants were randomized to receive either REGN-EB3 or Mab114, while remdesivir and ZMapp were no longer offered in the trial.[47] Mortality was 33.5% in the REGN-EB3 group, 35.1% in the Mab114 group, 49.7% in the ZMapp group, and 53.1% in the remdesivir group.[47]

In the trial, mortality at 28 days was 35.1% in patients treated with ansuvirimab, 33.5% in the REGN-EB3 group, compared to 49.7% in the ZMapp group.[47] There was no significant difference in mortality between remdesivir and ZMapp.[47]

Prognosis

The recovery rate of Ebola virus depends on early intervention and access to adequate healthcare with continuous supportive care and close-interval patient reassessment. Supportive care is essential to correct dehydration, anemia, and respiratory support if needed. Even with optimal treatment, the mortality rate remains high. Fatality rates vary depending on the outbreak: the earliest outbreak in 1976 had an 88% mortality rate for EBOV and 60% for SUDV, while more recent outbreaks have shown fatality rates as low as 40%, likely reflecting improved supportive care.[21]

Complications

The main complications caused by the Ebola virus are profound hypovolemia, hemorrhage, and multisystem organ failure, leading to shock and death.[1] Psychiatric illness is common in EVD survivors.[51] Most survivors experience the trauma of watching others die in ETUs and may sense reluctance of healthcare workers to provide care due to concerns about contracting the virus.[51]

Due to prolonged viral presence in semen and known sexual transmission, the World Health Organization recommends semen Ebola RT-PCR testing monthly starting 3 months after infection, with condom use or abstinence until 2 consecutive tests are negative at least one week apart.[18]

Deterrence and Patient Education

Close contacts should be educated about:

The disease's signs, symptoms, and expected progression.
Quarantine instructions, with the importance of strict adherence.
When to go to the hospital and the importance of Ebola treatment units (where available).
The importance of isolation of sick family members.
The risk of viral shedding through semen after recovery and the importance of safe sex practices or abstinence until semen tests negative for the virus.

Public engagement and education are vital to limit the number of cases spread in the community. Public Health education includes recognition of the signs and symptoms of EVD and understanding of the transmission of Ebola virus (ie, bodily fluids, sexual contact, objects, cadavers). In affected African countries, especially in rural areas, the dangers of eating bushmeat and identification, reporting of findings of dead or diseased animals, and the importance of bringing ill family members to healthcare services, should also be a part of routine public education. Community members will only implement these measures in an environment of trust; this is built through community engagement, explaining interventions and actions, and answering all questions.[1]

Enhancing Healthcare Team Outcomes

Ebola virus disease is of serious public health concern. Ebola virus is one of the world's deadliest pathogens and is difficult to contain. If it were not for the remote and rural locations of outbreaks, the risk of an Ebola pandemic would be more eminent. The 2013 to 2016 Ebolavirus epidemic highlighted the global threat of neglected tropical diseases.

Supportive care involving an interprofessional team remains the determining factor for patient prognosis and outcome. Adjunct therapy with monoclonal antibodies and antivirals successfully reduced mortality from EVD and must be widely available in affected areas. Early detection of Ebola virus disease by primary care providers, diligence in the isolation of suspected patients, and careful use of PPE to contain the spread of the Ebola virus are vital. Early involvement of the Infection Prevention and Control team and local or state health departments is a cornerstone of management. Establishing temporary or permanent Ebola virus disease treatment units is necessary, depending on the location.

(Click Image to Enlarge)

Ebola Virus

Contributed by S Bhimji, MD

Details

References

[1]

Feldmann H, Sprecher A, Geisbert TW. Ebola. The New England journal of medicine. 2020 May 7:382(19):1832-1842. doi: 10.1056/NEJMra1901594. Epub [PubMed PMID: 32441897]

[2]

Dixon MG, Schafer IJ, Centers for Disease Control and Prevention (CDC). Ebola viral disease outbreak--West Africa, 2014. MMWR. Morbidity and mortality weekly report. 2014 Jun 27:63(25):548-51 [PubMed PMID: 24964881]

[3]

Jacob ST, Crozier I, Fischer WA 2nd, Hewlett A, Kraft CS, Vega MA, Soka MJ, Wahl V, Griffiths A, Bollinger L, Kuhn JH. Ebola virus disease. Nature reviews. Disease primers. 2020 Feb 20:6(1):13. doi: 10.1038/s41572-020-0147-3. Epub 2020 Feb 20 [PubMed PMID: 32080199]

[4]

Khan S, Muhammad, Rauf A, Khan A, Rizwan M, Patel S, Khan H, Mahasneh AM, Mubarak MS. Comprehensive Review on Ebola (EBOV) Virus: Future Prospects. Infectious disorders drug targets. 2018:18(2):96-104. doi: 10.2174/1871526517666170817100828. Epub [PubMed PMID: 28820067]

[5]

Emanuel J, Marzi A, Feldmann H. Filoviruses: Ecology, Molecular Biology, and Evolution. Advances in virus research. 2018:100():189-221. doi: 10.1016/bs.aivir.2017.12.002. Epub 2018 Feb 1 [PubMed PMID: 29551136]

Level 3 (low-level) evidence

[6]

Hayman DT, Yu M, Crameri G, Wang LF, Suu-Ire R, Wood JL, Cunningham AA. Ebola virus antibodies in fruit bats, Ghana, West Africa. Emerging infectious diseases. 2012 Jul:18(7):1207-9. doi: 10.3201/eid1807.111654. Epub [PubMed PMID: 22710257]

[7]

Letafati A, Salahi Ardekani O, Karami H, Soleimani M. Ebola virus disease: A narrative review. Microbial pathogenesis. 2023 Aug:181():106213. doi: 10.1016/j.micpath.2023.106213. Epub 2023 Jun 23 [PubMed PMID: 37355146]

Level 3 (low-level) evidence

[8]

Lacroix A, Mbala Kingebeni P, Ndimbo Kumugo SP, Lempu G, Butel C, Serrano L, Vidal N, Thaurignac G, Esteban A, Mukadi Bamuleka D, Likofata J, Delaporte E, Muyembe Tamfum JJ, Ayouba A, Peeters M, Ahuka Mundeke S. Investigating the Circulation of Ebola Viruses in Bats during the Ebola Virus Disease Outbreaks in the Equateur and North Kivu Provinces of the Democratic Republic of Congo from 2018. Pathogens (Basel, Switzerland). 2021 May 4:10(5):. doi: 10.3390/pathogens10050557. Epub 2021 May 4 [PubMed PMID: 34064424]

[9]

Negredo A, Palacios G, Vázquez-Morón S, González F, Dopazo H, Molero F, Juste J, Quetglas J, Savji N, de la Cruz Martínez M, Herrera JE, Pizarro M, Hutchison SK, Echevarría JE, Lipkin WI, Tenorio A. Discovery of an ebolavirus-like filovirus in europe. PLoS pathogens. 2011 Oct:7(10):e1002304. doi: 10.1371/journal.ppat.1002304. Epub 2011 Oct 20 [PubMed PMID: 22039362]

[10]

Broadhurst MJ, Brooks TJ, Pollock NR. Diagnosis of Ebola Virus Disease: Past, Present, and Future. Clinical microbiology reviews. 2016 Oct:29(4):773-93. doi: 10.1128/CMR.00003-16. Epub [PubMed PMID: 27413095]

[11]

Tomori O, Kolawole MO. Ebola virus disease: current vaccine solutions. Current opinion in immunology. 2021 Aug:71():27-33. doi: 10.1016/j.coi.2021.03.008. Epub 2021 Apr 17 [PubMed PMID: 33873076]

Level 3 (low-level) evidence

[12]

Barbiero VK. Ebola: A Hyperinflated Emergency. Global health, science and practice. 2020 Jun 30:8(2):178-182. doi: 10.9745/GHSP-D-19-00422. Epub 2020 Jun 30 [PubMed PMID: 32430358]

[13]

Baudel H, De Nys H, Mpoudi Ngole E, Peeters M, Desclaux A. Understanding Ebola virus and other zoonotic transmission risks through human-bat contacts: Exploratory study on knowledge, attitudes and practices in Southern Cameroon. Zoonoses and public health. 2019 May:66(3):288-295. doi: 10.1111/zph.12563. Epub 2019 Jan 24 [PubMed PMID: 30677236]

Level 3 (low-level) evidence

[14]

Nkoghe D, Formenty P, Leroy EM, Nnegue S, Edou SY, Ba JI, Allarangar Y, Cabore J, Bachy C, Andraghetti R, de Benoist AC, Galanis E, Rose A, Bausch D, Reynolds M, Rollin P, Choueibou C, Shongo R, Gergonne B, Koné LM, Yada A, Roth C, Mve MT. [Multiple Ebola virus haemorrhagic fever outbreaks in Gabon, from October 2001 to April 2002]. Bulletin de la Societe de pathologie exotique (1990). 2005 Sep:98(3):224-9 [PubMed PMID: 16267965]

[15]

Bisimwa P, Biamba C, Aborode AT, Cakwira H, Akilimali A. Ebola virus disease outbreak in the Democratic Republic of the Congo: A mini-review. Annals of medicine and surgery (2012). 2022 Aug:80():104213. doi: 10.1016/j.amsu.2022.104213. Epub 2022 Jul 20 [PubMed PMID: 35875058]

[16]

Cenciarelli O, Gabbarini V, Pietropaoli S, Malizia A, Tamburrini A, Ludovici GM, Carestia M, Di Giovanni D, Sassolini A, Palombi L, Bellecci C, Gaudio P. Viral bioterrorism: Learning the lesson of Ebola virus in West Africa 2013-2015. Virus research. 2015 Dec 2:210():318-26. doi: 10.1016/j.virusres.2015.09.002. Epub 2015 Sep 8 [PubMed PMID: 26359111]

[17]

Uyeki TM, Erickson BR, Brown S, McElroy AK, Cannon D, Gibbons A, Sealy T, Kainulainen MH, Schuh AJ, Kraft CS, Mehta AK, Lyon GM 3rd, Varkey JB, Ribner BS, Ellison RT 3rd, Carmody E, Nau GJ, Spiropoulou C, Nichol ST, Ströher U. Ebola Virus Persistence in Semen of Male Survivors. Clinical infectious diseases : an official publication of the Infectious Diseases Society of America. 2016 Jun 15:62(12):1552-1555. doi: 10.1093/cid/ciw202. Epub 2016 Apr 3 [PubMed PMID: 27045122]

[18]

Fischer WA 2nd, Wohl DA. Confronting Ebola as a Sexually Transmitted Infection. Clinical infectious diseases : an official publication of the Infectious Diseases Society of America. 2016 May 15:62(10):1272-6. doi: 10.1093/cid/ciw123. Epub 2016 Mar 1 [PubMed PMID: 26936667]

[19]

Maxmen A. Ebola outbreak declared an international public-health emergency. Nature. 2019 Jul 17:():. doi: 10.1038/d41586-019-02221-3. Epub 2019 Jul 17 [PubMed PMID: 32669721]

[20]

Curran KG, Gibson JJ, Marke D, Caulker V, Bomeh J, Redd JT, Bunga S, Brunkard J, Kilmarx PH. Cluster of Ebola Virus Disease Linked to a Single Funeral - Moyamba District, Sierra Leone, 2014. MMWR. Morbidity and mortality weekly report. 2016 Mar 4:65(8):202-5. doi: 10.15585/mmwr.mm6508a2. Epub 2016 Mar 4 [PubMed PMID: 26938950]

[21]

Baseler L, Chertow DS, Johnson KM, Feldmann H, Morens DM. The Pathogenesis of Ebola Virus Disease. Annual review of pathology. 2017 Jan 24:12():387-418. doi: 10.1146/annurev-pathol-052016-100506. Epub [PubMed PMID: 27959626]

[22]

Zawilińska B, Kosz-Vnenchak M. General introduction into the Ebola virus biology and disease. Folia medica Cracoviensia. 2014:54(3):57-65 [PubMed PMID: 25694096]

[23]

Leroy EM, Gonzalez JP, Baize S. Ebola and Marburg haemorrhagic fever viruses: major scientific advances, but a relatively minor public health threat for Africa. Clinical microbiology and infection : the official publication of the European Society of Clinical Microbiology and Infectious Diseases. 2011 Jul:17(7):964-76. doi: 10.1111/j.1469-0691.2011.03535.x. Epub [PubMed PMID: 21722250]

Level 3 (low-level) evidence

[24]

Marshall Lyon G, Mehta AK, Ribner BS. Clinical Management of Patients with Ebola Virus Disease in High-Resource Settings. Current topics in microbiology and immunology. 2017:411():115-137. doi: 10.1007/82_2017_19. Epub [PubMed PMID: 28601946]

[25]

Lamontagne F, Fowler RA, Adhikari NK, Murthy S, Brett-Major DM, Jacobs M, Uyeki TM, Vallenas C, Norris SL, Fischer WA 2nd, Fletcher TE, Levine AC, Reed P, Bausch DG, Gove S, Hall A, Shepherd S, Siemieniuk RA, Lamah MC, Kamara R, Nakyeyune P, Soka MJ, Edwin A, Hazzan AA, Jacob ST, Elkarsany MM, Adachi T, Benhadj L, Clément C, Crozier I, Garcia A, Hoffman SJ, Guyatt GH. Evidence-based guidelines for supportive care of patients with Ebola virus disease. Lancet (London, England). 2018 Feb 17:391(10121):700-708. doi: 10.1016/S0140-6736(17)31795-6. Epub 2017 Oct 17 [PubMed PMID: 29054555]

Level 1 (high-level) evidence

[26]

Mérens A, Bigaillon C, Delaune D. Ebola virus disease: Biological and diagnostic evolution from 2014 to 2017. Medecine et maladies infectieuses. 2018 Mar:48(2):83-94. doi: 10.1016/j.medmal.2017.11.002. Epub 2017 Dec 8 [PubMed PMID: 29224715]

[27]

Southern TR, Racsa LD, Albariño CG, Fey PD, Hinrichs SH, Murphy CN, Herrera VL, Sambol AR, Hill CE, Ryan EL, Kraft CS, Campbell S, Sealy TK, Schuh A, Ritchie JC, Lyon GM 3rd, Mehta AK, Varkey JB, Ribner BS, Brantly KP, Ströher U, Iwen PC, Burd EM. Comparison of FilmArray and Quantitative Real-Time Reverse Transcriptase PCR for Detection of Zaire Ebolavirus from Contrived and Clinical Specimens. Journal of clinical microbiology. 2015 Sep:53(9):2956-60. doi: 10.1128/JCM.01317-15. Epub 2015 Jul 8 [PubMed PMID: 26157148]

[28]

Muzembo BA, Kitahara K, Ohno A, Ntontolo NP, Ngatu NR, Okamoto K, Miyoshi SI. Rapid diagnostic tests versus RT-PCR for Ebola virus infections: a systematic review and meta-analysis. Bulletin of the World Health Organization. 2022 Jul 1:100(7):447-458. doi: 10.2471/BLT.21.287496. Epub 2022 Jun 1 [PubMed PMID: 35813519]

Level 1 (high-level) evidence

[29]

Moran Z, Rodriguez W, Ahmadou D, Soropogui B, Magassouba NF, Kelly-Cirino C, Ben Amor Y. Comparative performance study of three Ebola rapid diagnostic tests in Guinea. BMC infectious diseases. 2020 Sep 15:20(1):670. doi: 10.1186/s12879-020-05339-2. Epub 2020 Sep 15 [PubMed PMID: 32933492]

Level 2 (mid-level) evidence

[30]

Coarsey CT, Esiobu N, Narayanan R, Pavlovic M, Shafiee H, Asghar W. Strategies in Ebola virus disease (EVD) diagnostics at the point of care. Critical reviews in microbiology. 2017 Nov:43(6):779-798. doi: 10.1080/1040841X.2017.1313814. Epub 2017 Apr 25 [PubMed PMID: 28440096]

[31]

Vogl TJ, Martin S, Brodt HR, Keppler O, Zacharowski K, Wolf T. The Frankfurt Ebola patient. RoFo : Fortschritte auf dem Gebiete der Rontgenstrahlen und der Nuklearmedizin. 2015 Sep:187(9):771-6. doi: 10.1055/s-0035-1553130. Epub 2015 Jun 19 [PubMed PMID: 26090732]

[32]

Althaus CL. Estimating the Reproduction Number of Ebola Virus (EBOV) During the 2014 Outbreak in West Africa. PLoS currents. 2014 Sep 2:6():. pii: ecurrents.outbreaks.91afb5e0f279e7f29e7056095255b288. doi: 10.1371/currents.outbreaks.91afb5e0f279e7f29e7056095255b288. Epub 2014 Sep 2 [PubMed PMID: 25642364]

[33]

Biedron C, Lyman M, Stuckey MJ, Homsy J, Lamorde M, Luvsansharav UO, Wilson K, Gomes D, Omuut W, Okware S, Semanda JN, Kiggundu R, Bulwadda D, Brown V, Nelson LJ, Driwale A, Fagan R, Park BJ, Smith RM. Evaluation of Infection Prevention and Control Readiness at Frontline Health Care Facilities in High-Risk Districts Bordering Ebola Virus Disease-Affected Areas in the Democratic Republic of the Congo - Uganda, 2018. MMWR. Morbidity and mortality weekly report. 2019 Oct 4:68(39):851-854. doi: 10.15585/mmwr.mm6839a4. Epub 2019 Oct 4 [PubMed PMID: 31581162]

[34]

Bell BP, Damon IK, Jernigan DB, Kenyon TA, Nichol ST, O'Connor JP, Tappero JW. Overview, Control Strategies, and Lessons Learned in the CDC Response to the 2014-2016 Ebola Epidemic. MMWR supplements. 2016 Jul 8:65(3):4-11. doi: 10.15585/mmwr.su6503a2. Epub 2016 Jul 8 [PubMed PMID: 27389903]

Level 3 (low-level) evidence

[35]

Cummings KJ, Choi MJ, Esswein EJ, de Perio MA, Harney JM, Chung WM, Lakey DL, Liddell AM, Rollin PE. Addressing Infection Prevention and Control in the First U.S. Community Hospital to Care for Patients With Ebola Virus Disease: Context for National Recommendations and Future Strategies. Annals of internal medicine. 2016:165(1):41-49. doi: 10.7326/M15-2944. Epub 2016 May 10 [PubMed PMID: 27159355]

[36]

Verbeek JH, Rajamaki B, Ijaz S, Sauni R, Toomey E, Blackwood B, Tikka C, Ruotsalainen JH, Kilinc Balci FS. Personal protective equipment for preventing highly infectious diseases due to exposure to contaminated body fluids in healthcare staff. The Cochrane database of systematic reviews. 2020 May 15:5(5):CD011621. doi: 10.1002/14651858.CD011621.pub5. Epub 2020 May 15 [PubMed PMID: 32412096]

Level 1 (high-level) evidence

[37]

Shenoy ES, Weber DJ. Lessons learned in infection prevention for Ebola virus disease and the coronavirus disease 2019 (COVID-19) pandemic-Principles underlying prevention. Infection control and hospital epidemiology. 2021 Apr:42(4):457-460. doi: 10.1017/ice.2020.1427. Epub 2021 Jan 11 [PubMed PMID: 33427132]

[38]

Bogoch II, Creatore MI, Cetron MS, Brownstein JS, Pesik N, Miniota J, Tam T, Hu W, Nicolucci A, Ahmed S, Yoon JW, Berry I, Hay SI, Anema A, Tatem AJ, MacFadden D, German M, Khan K. Assessment of the potential for international dissemination of Ebola virus via commercial air travel during the 2014 west African outbreak. Lancet (London, England). 2015 Jan 3:385(9962):29-35. doi: 10.1016/S0140-6736(14)61828-6. Epub 2014 Oct 21 [PubMed PMID: 25458732]

[39]

Nuzzo JB, Cicero AJ, Waldhorn R, Inglesby TV. Travel bans will increase the damage wrought by ebola. Biosecurity and bioterrorism : biodefense strategy, practice, and science. 2014 Nov-Dec:12(6):306-9. doi: 10.1089/bsp.2014.1030. Epub [PubMed PMID: 25397355]

[40]

Hunt L, Gupta-Wright A, Simms V, Tamba F, Knott V, Tamba K, Heisenberg-Mansaray S, Tamba E, Sheriff A, Conteh S, Smith T, Tobin S, Brooks T, Houlihan C, Cummings R, Fletcher T. Clinical presentation, biochemical, and haematological parameters and their association with outcome in patients with Ebola virus disease: an observational cohort study. The Lancet. Infectious diseases. 2015 Nov:15(11):1292-9. doi: 10.1016/S1473-3099(15)00144-9. Epub 2015 Aug 10 [PubMed PMID: 26271406]

[41]

Kaplon H, Reichert JM. Antibodies to watch in 2021. mAbs. 2021 Jan-Dec:13(1):1860476. doi: 10.1080/19420862.2020.1860476. Epub [PubMed PMID: 33459118]

[42]

Taki E, Ghanavati R, Navidifar T, Dashtbin S, Heidary M, Moghadamnia M. Ebanga™: The most recent FDA-approved drug for treating Ebola. Frontiers in pharmacology. 2023:14():1083429. doi: 10.3389/fphar.2023.1083429. Epub 2023 Mar 8 [PubMed PMID: 36969842]

[43]

Markham A. REGN-EB3: First Approval. Drugs. 2021 Jan:81(1):175-178. doi: 10.1007/s40265-020-01452-3. Epub [PubMed PMID: 33432551]

[44]

Wong G. Progress in Elucidating Potential Markers and Mechanisms of Rapid Protection Conferred by the VSV-Vectored Ebola Virus Vaccine. mBio. 2019 Jul 16:10(4):. doi: 10.1128/mBio.01597-19. Epub 2019 Jul 16 [PubMed PMID: 31311887]

[45]

PREVAC Study Team, Kieh M, Richert L, Beavogui AH, Grund B, Leigh B, D'Ortenzio E, Doumbia S, Lhomme E, Sow S, Vatrinet R, Roy C, Kennedy SB, Faye S, Lees S, Millimouno NP, Camara AM, Samai M, Deen GF, Doumbia M, Espérou H, Pierson J, Watson-Jones D, Diallo A, Wentworth D, McLean C, Simon J, Wiedemann A, Dighero-Kemp B, Hensley L, Lane HC, Levy Y, Piot P, Greenwood B, Chêne G, Neaton J, Yazdanpanah Y. Randomized Trial of Vaccines for Zaire Ebola Virus Disease. The New England journal of medicine. 2022 Dec 29:387(26):2411-2424. doi: 10.1056/NEJMoa2200072. Epub 2022 Dec 14 [PubMed PMID: 36516078]

Level 1 (high-level) evidence

[46]

PREVAIL II Writing Group, Multi-National PREVAIL II Study Team, Davey RT Jr, Dodd L, Proschan MA, Neaton J, Neuhaus Nordwall J, Koopmeiners JS, Beigel J, Tierney J, Lane HC, Fauci AS, Massaquoi MBF, Sahr F, Malvy D. A Randomized, Controlled Trial of ZMapp for Ebola Virus Infection. The New England journal of medicine. 2016 Oct 13:375(15):1448-1456 [PubMed PMID: 27732819]

Level 1 (high-level) evidence

[47]

Mulangu S, Dodd LE, Davey RT Jr, Tshiani Mbaya O, Proschan M, Mukadi D, Lusakibanza Manzo M, Nzolo D, Tshomba Oloma A, Ibanda A, Ali R, Coulibaly S, Levine AC, Grais R, Diaz J, Lane HC, Muyembe-Tamfum JJ, PALM Writing Group, Sivahera B, Camara M, Kojan R, Walker R, Dighero-Kemp B, Cao H, Mukumbayi P, Mbala-Kingebeni P, Ahuka S, Albert S, Bonnett T, Crozier I, Duvenhage M, Proffitt C, Teitelbaum M, Moench T, Aboulhab J, Barrett K, Cahill K, Cone K, Eckes R, Hensley L, Herpin B, Higgs E, Ledgerwood J, Pierson J, Smolskis M, Sow Y, Tierney J, Sivapalasingam S, Holman W, Gettinger N, Vallée D, Nordwall J, PALM Consortium Study Team. A Randomized, Controlled Trial of Ebola Virus Disease Therapeutics. The New England journal of medicine. 2019 Dec 12:381(24):2293-2303. doi: 10.1056/NEJMoa1910993. Epub 2019 Nov 27 [PubMed PMID: 31774950]

Level 1 (high-level) evidence

[48]

Pardo J, Shukla AM, Chamarthi G, Gupte A. The journey of remdesivir: from Ebola to COVID-19. Drugs in context. 2020:9():. doi: 10.7573/dic.2020-4-14. Epub 2020 May 22 [PubMed PMID: 32547625]

[49]

Malin JJ, Suárez I, Priesner V, Fätkenheuer G, Rybniker J. Remdesivir against COVID-19 and Other Viral Diseases. Clinical microbiology reviews. 2020 Dec 16:34(1):. doi: 10.1128/CMR.00162-20. Epub 2020 Oct 14 [PubMed PMID: 33055231]

[50]

Qiu X, Wong G, Audet J, Bello A, Fernando L, Alimonti JB, Fausther-Bovendo H, Wei H, Aviles J, Hiatt E, Johnson A, Morton J, Swope K, Bohorov O, Bohorova N, Goodman C, Kim D, Pauly MH, Velasco J, Pettitt J, Olinger GG, Whaley K, Xu B, Strong JE, Zeitlin L, Kobinger GP. Reversion of advanced Ebola virus disease in nonhuman primates with ZMapp. Nature. 2014 Oct 2:514(7520):47-53. doi: 10.1038/nature13777. Epub 2014 Aug 29 [PubMed PMID: 25171469]

Level 2 (mid-level) evidence

[51]

Tucci V, Moukaddam N, Meadows J, Shah S, Galwankar SC, Kapur GB. The Forgotten Plague: Psychiatric Manifestations of Ebola, Zika, and Emerging Infectious Diseases. Journal of global infectious diseases. 2017 Oct-Dec:9(4):151-156. doi: 10.4103/jgid.jgid_66_17. Epub [PubMed PMID: 29302150]