The document discusses the 2014-2016 Ebola virus outbreak in West Africa, the largest and most complex Ebola outbreak in history. Key points:
- The outbreak was declared a Public Health Emergency of International Concern by the WHO in August 2014 due to the high risks of international spread.
- Factors exacerbating the outbreak included widespread transmission in communities and healthcare settings, weak infrastructure in affected countries, and lack of knowledge about the disease leading to unsafe practices.
- The outbreak had massive social and economic impacts on the affected regions through disruption of industries, increased poverty, orphaning of children, and lack of access to healthcare for other conditions.
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Ebola Seminar
1.
2. Prototype Viral
Hemorrhagic Fever
Pathogen
Filovirus:enveloped,
non-segmented, negative-
stranded RNA virus
Severe disease with high
case fatality
Absence of specific
treatment or vaccine
>20 previous Ebola and
Marburg virus outbreaks
2014 West Africa Ebola
outbreak caused by
Zaire ebolavirus species
(five known Ebola virus
species)
3. First appeared in Africa 1976
“African Hemorrhagic Fever”
acute, mostly fatal disease
causes blood vessel “bursting”
systemic (all organs/tissues)
humans and nonhuman primates
Excluding 2000 outbreak
1,500 cases
over 1,000 deaths
6. 2002- Fruit Bats
Antibodies against
Ebola
Ebola Gene sequences
in liver and spleen
Fruit bats do not show
any symptoms
Best candidate to be
the reservoir
More research needs to
be done
7. The link between human infection by the Ebola
virus and their proximity to primates is clear.
-Outbreaks occurred in countries that house 80
percent of the world’s remaining wild gorilla and
chimpanzee populations.
- The outbreaks coincided with the outbreaks in
wild animals.
- The same distinct viral strains were isolated in
animal carcasses and in the bodies of those who
handled those carcasses.
- These outbreaks were preceded by an
abnormally high death reports in wild Gorilla
populations.
8.
9. Country
Reporting
Date
Total Cases
Confirmed
Cases
Total Deaths
Guinea 27 Oct 14 1,906 1,391 997
Liberia 25 Oct 14 6,535 2,515 2,413
Sierra Leone 27 Oct 14 5,235 3,700 1,500
Nigeria** 15 Oct 14 20 19 8
Spain 27 Oct 14 1 1 0
Senegal** 15 Oct 14 1 1 0
United
States
24 Oct 14 4 4 1
Mali 23 Oct 14 1 1 1
TOTAL 13,733 7,632 4,920
10. Virus present in high quantity in blood, body fluids,
and excreta of symptomatic EVD-infected patients
Opportunities for human-to-human transmission
Direct contact (through broken skin or unprotected mucous
membranes) with an EVD-infected patient’s blood or body
fluids
Sharps injury (with EVD-contaminated needle or other
sharp)
Direct contact with the corpse of a person who died of EVD
Indirect contact with an EVD-infected patient’s blood or
body fluids via a contaminated object (soiled linens or used
utensils)
Ebola can also be transmitted via contact with blood,
fluids, or meat of an infected animal
11. Infected persons are not contagious until onset of
symptoms
Infectiousness of body fluids (e.g., viral load)
increases as patient becomes more ill
Remains from deceased infected persons are highly
infectious
Human-to-human transmission of Ebola virus via
inhalation (aerosols) has not been demonstrated
12. Direct infection of tissues
Immune dysregulation
Hypovolemia and vascular
collapse
Electrolyte abnormalities
Multi-organ failure, septic
shock
Disseminated intravascular
coagulation (DIC) and
coagulopathy
13. Other possible infectious causes of symptoms: (Differential Diagnosis)
Malaria, typhoid fever, meningococcemia, Lassa fever and other
bacterial infections like pneumonia which are all very common in Africa.
14.
15. Incubation period: 2-21 days
Stage I (unspecific):
-Extreme asthenia (body weakness)
-diarrhea, nausea and vomiting, anorexia
abdominal pain
- headaches
- arthralgia (neuralgic pain in joints)
- myalgia (muscular pain or tenderness), back pain
- mucosal redness of the oral cavity, dysphagia (difficulty
in swallowing)
- conjunctivitis.
- rash all over body except in face
** If the patients don’t recover gradually at this point, there is a high
probability that the disease will progress to the second phase,
resulting in complications which eventually lead to death (Mupapa et
al., 1999).
16. Stage II (Specific):
- Hemorrhage
- neuropsychiatric abnormalities
- anuria (the absence of urine formation)
- hiccups
- tachypnea (rapid breathing).
** Patients who progressed to phase two EHF almost
always die. (Ndambi et al., 1999)
Late Complications:
-Arthralgia
- ocular diseases (ocular pain, photophobia and
hyperlacrimation)
- hearing loss
- unilateral orchitis( inflammation of one or both of the
testes)
** These conditions are usually relieved with the treatment
of 1% atropine and steroids
17. Nonspecific early symptoms progress to:
Hypovolemic shock and multi-organ failure
Hemorrhagic disease
Death
Non-fatal cases typically improve 6–11 days after
symptoms onset
Fatal disease associated with more severe early
symptoms
Fatality rates of 70% have been reported in rural Africa
Intensive care, especially early intravenous and
electrolyte management, may increase the survival rate
19. Thrombocytopenia (50,000–100,000/mL range)
Leukopenia followed by neutrophilia
Transaminase elevation: elevation serum aspartate
amino-transferase (AST) > alanine transferase (ALT)
Electrolyte abnormalities from fluid shifts
Coagulation: PT and PTT prolonged
Renal: proteinuria, increased creatinine
20. Timeline of infection Diagnostic tests available
Within a few days after onset Antigen-capture enzyme-
linked immunosorbent assay
(ELISA) testing
IgM ELISA
Polymerase chain reaction
(PCR)
Virus isolation
Later in disease course or after
recovery
Serology: IgM and IgG
Retrospectively in deceased
patients
Immunohistochemistry testing
PCR
Virus isolation
21.
22. Hypovolemia and Sepsis Physiology
Aggressive intravenous fluid resuscitation
Hemodynamic support and critical care management if
necessary
Electrolyte and acid-base abnormalities
Aggressive electrolyte repletion
Correction of acid-base derangements
Symptomatic management of fever and
gastrointestinal symptoms
Avoid NSAIDS
Multisystem organ failure can develop and may
require
Oxygenation and mechanical ventilation in ICU settings
Correction of severe coagulopathy
Renal replacement therapy
23. No approved Ebola-specific prophylaxis or treatment
Ribavirin has no in-vitro or in-vivo effect on Ebola virus
Therapeutics in development with limited human clinical trial
data
• Convalescent serum
• Therapeutic medications
o Zmapp – chimeric human-mouse monoclonal antibodies
o Tekmira – lipid nanoparticle small interfering RNA
o Brincidofovir – oral nucleotide analogue with antiviral
activity
Vaccines – in clinical trials
• Chimpanzee-derived adenovirus with an Ebola virus gene
inserted
• Attenuated vesicular stomatitis virus with an Ebola virus
gene inserted
24. Case-fatality rate 71% in the 2014 Ebola outbreak
Case-fatality rate is likely much lower with access to intensive
care
Patients who survive often have signs of clinical
improvement by the second week of illness
Associated with the development of virus-specific antibodies
Antibody with neutralizing activity against Ebola persists
greater than 12 years after infection
Prolonged convalescence
Includes arthralgia, myalgia, abdominal pain, extreme fatigue,
and anorexia; many symptoms resolve by 21 months
Significant arthralgia and myalgia may persist for >21 months
Skin sloughing and hair loss has also been reported
25. The world is currently facing the biggest and most complex
Ebola outbreak in history. On August 8, 2014, the Ebola
outbreak in West Africa was declared by the World Health
Organization (WHO) to be a Public Health Emergency of
International Concern (PHEIC) because it was determined to be
an "extraordinary event" with public health risks to other
countries. The possible consequences of further international
spread are particularly serious considering the following
factors:
The virulence (ability to cause serious disease or death) of
the virus.
The widespread transmission in communities and healthcare
facilities in the currently affected countries and
The strained health systems in the currently affected and
most at-risk countries.
PHIEC
26. •Widespread on multiple fronts
•Affected large cities
•Weak and fragile infrastructure
•Lack of knowledge of the disease
•Distrust of government and foreigners
•Not seeking voluntary health care
•Social rituals / burial rituals
•Delayed response; more resources needed
Context for outbreak
27. Impact on social determinants of health
Trading, industry, agriculture, tourism
Worsening poverty
Hunger
Orphans
Stigma
School closures
Other diseases not being treated
Lack of preventive care: prenatal care, vaccination
28. Bio-geographical Ethics is defined as
motivation based on ideas of right and wrong
when dealing with the geographical distribution
of animals and plants.
This concept of can be used to explain the
world’s shockingly small response to the Ebola
Virus.
As there was little travel to that region by
people of more developed countries, there was
not much economic drive for a vaccine,
treatment and aid in prevention.
The Ebola Virus is now however on the “A” list
for hopeful vaccination development.
Experiments have even been formed to show
how Ebola can be used as a bioterror agent.
29.
30. RISK LEVEL PUBLIC HEALTH ACTION
Monitoring Restricted
Public Activities
Restricted
Travel
HIGH risk
Direct Active
Monitoring
Yes Yes
SOME risk
Direct Active
Monitoring
Case-by-
case
assessment
Case-by-
case
assessment
LOW risk
Active Monitoring
for some;
Direct Active
Monitoring
for others
No No
NO risk No No No