Title: BIODEFENSE
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BIODEFENSE Epidemiology of Anthrax Shahid
Beheshti University of medical sciences,
2007 By Hatami H. MD. MPH
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- Human zoonotic disease
- Primarily disease of herbivorous animals
- Sheep, goats, cattle
- Many large documented epizootics
- Occasional human disease
- Epidemics have occurred but uncommon
- Rare in developed world
4Bioweapon Potential
- Many countries have weaponized anthrax
- Former bioweapon programs
- U.S.S.R., U.S., U.K., and Japan
- Recent bioweapon programs
- Iraq
- Attempted uses as bioterrorism agent
- WW I Germans inoculated Allied livestock
- WW II Japanese use on prisoners
5Bioweapon Potential
- Features of anthrax suitable as BT agent
- Spores easily dispersed as aerosol
- Moderately infectious
- High mortality for inhalational (86-100)
- Fairly easy to obtain, produce and store
6Bioweapon Potential
- Aerosol method of delivery
- Most likely method expected in BT attack
- Would cause primarily inhalational disease
- Spores reside on particles of 1-5 µm size
- Optimal size for deposition into alveoli
- Form of disease with highest mortality
- Would infect the largest number of people
7Bioweapon Potential
- Sverdlovsk, Russia 1979
- Accidental release from anthrax drying plant
- 79 human cases
- All downwind of plant
- 68 deaths
- Some infected with multiples strains
8Bioweapon Potential
- Estimated effects of inhalational anthrax
- 100 kg spores released over city size of
Washington DC - 130,000 3 million deaths depending on weather
conditions - Economic impact
- 26.2 billion/100,000 exposed people
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period of communicability)
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- Incubation Period
- Time from exposure to symptoms
- Cutaneous, 3-10 days
- Very variable for inhalational
- 2-43 days reported
- Theoretically may be up to 100 days
- Delayed germination of spores
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- Caused by Bacillus anthracis
- Spores found in soil worldwide
- Bacillus anthracis
- Aerobic, Gram positive rod
- Long (1-10µm), thin (0.5-2.5µm)
- Forms inert spores when exposed to O2
- Infectious form, hardy
- Approx 1µm in size
- Vegetative bacillus state in vivo
- Result of spore germination
- Non-infectious, fragile
12- Environmental Survival
- Spores are hardy
- Resistant to drying, boiling lt10 minutes
- Survive for years in soil
- Still viable for decades in perma-frost
- Favorable soil factors for spore viability
- High moisture
- Organic content
- Alkaline pH
- High calcium concentration
13- Protective Antigen
- Binds Edema Factor to form Edema Toxin
- Facilitates entry of Edema Toxin into cells
- Edema Factor
- Massive edema by increasing intracellular cAMP
- Also inhibits neutrophil function
- Lethal Factor
- Stimulates macrophage release of TNF-a, IL-1ß
- Initiates cascade of events leading to sepsis
14Pathogenesis
- Disease requires entry of spores into body
- Exposure does not always cause disease
- Inoculation dose
- Route of entry
- Host immune status
- May depend on pathogen strain characteristics
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- Three forms of natural disease
- Inhalational
- Rare (lt5)
- Most likely encountered in bioterrorism event
- Cutaneous
- Most common (95)
- Direct contact of spores on skin
- Gastrointestinal
- Rare (lt5),
- Ingestion
- Mortality
- Inhalational 86-100 (despite treatment)
- Era of crude intensive supportive care
- Cutaneous lt5 (treated) 20 (untreated)
- GI approaches 100
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??????? 85-1333
18Anthrax Disease Complex Summary
Inhalational
Tracheobronchial Lymphadenitis
Cutaneous
Mediastinitis, cyanosis, stridor, pulmonary edema
Hemorrhagic Meningitis
Papule vesicle, edema eschar
50
24 - 36 hours
20
Resolve
Toxic shock and Death
19Bioweapon Potential
- Inhalational
- Asymptomatic incubation period
- Duration 2-43 days, 10 days in Sverdlovsk
- Prodromal phase
- Correlates with germination, toxin production
- Nonspecific flu-like symptoms
- Fever, malaise, myalgias
- Dyspnea, nonproductive cough, mild chest
discomfort - Duration several hours to 3 days
- Can have transient resolution before next phase
- Fulminant Phase
20Clinical Features
- Inhalational
- Fulminant Phase
- Correlates with high-grade bacteremia/toxemia
- Critically Ill
- Fever, diaphoresis
- Respiratory distress/failure, cyanosis
- Septic shock, multiorgan failure, DIC
- 50 develop hemorrhagic meningitis
- Headache, meningismus, delirium, coma
- May be most prominent finding
- Usually progresses to death in lt36 hrs
- Mean time from symptom onset to death 3 days
21Clinical Features
- Laboratory Findings
- Gram positive bacilli in direct blood smear
- Electrolyte imbalances common
- Radiographic Findings
- Widened mediastinum
- Minimal or no infiltrates
- Can appear during prodrome phase
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23Clinical Features
- Cutaneous
- Most common areas of exposure
- Hands/arms
- Neck/head
- Incubation period
- 3-5 days typical
- 12 days maximum
24Clinical Features
- Cutaneous progression of painless lesions
- Papule pruritic
- Vesicle/bulla
- Ulcer contains organisms, sig. edema
- Eschar black, rarely scars
24-36 hrs
days
25Clinical Features
- Cutaneous
- Systemic disease may develop
- Lymphangitis and lymphadenopathy
- If untreated, can progress to sepsis, death
26Clinical Features
- Gastrointestinal
- Oropharyngeal
- Oral or esophageal ulcer
- Regional lymphadenopathy
- Edema, ascites
- Sepsis
- Abdominal
- Early symptoms - nausea, vomiting, malaise
- Late - hematochezia, acute abdomen, ascites
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- Occurs worldwide
- Endemic areas - Africa, Asia
- True incidence not known
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36Transmission
- Human cases historical risk factors
- Agricultural
- Exposure to livestock
- Occupational
- Exposure to wool and hides
- Woolsorters disease inhalational anthrax
- Rarely laboratory-acquired
37Transmission
38Transmission
- No human-to-human
- Naturally occurring cases
- Skin exposure
- Ingestion
- Airborne
- Bioterrorism
- Aerosol (likely)
- Small volume powder (possible)
- Foodborne (unlikely)
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- Primordial Prevention minimize hazards to
health - Primary Prevention
- Prevention of disease in well individuals
- Secondary Prevention
- Identification and intervention in early stages
of disease - Tertiary Prevention
- Prevention of further deterioration, reduction in
complications
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42- Vaccine
- Inactivated, cell-free filtrate
- Adsorbed onto Al(OH)3
- Protective Antigen
- Administration
- Dose schedule
- 0, 2 4 wks 6, 12 18 months initial series
- Annual booster
- 0.5 ml SQ
43- Vaccine
- Efficacy
- gt95 protection vs. aerosol in animal models
- gt90 vs. cutaneous in humans
44- Adverse Effects
- gt1.6 million doses given to military by 4/2000
- No deaths
- lt10 moderate/severe local reactions
- Erythema, edema
- lt1 systemic reactions
- Fever, malaise
45Postexposure Prophylaxis
- Who should receive PEP?
- Anyone exposed to anthrax
- Empiric antibiotic therapy
- Vaccination
- Not for contacts of cases, unless also exposed
46Postexposure Prophylaxis
- Avoid unnecessary antibiotic usage
- Potential shortages of those who need them
- Potential adverse effects
- Hypersensitivity
- Neurological side effects, especially elderly
- Bone/cartilage disease in children
- Oral contraceptive failure
- Future antibiotic resistance
- Individuals own flora
- Community resistance patterns
47Postexposure Prophylaxis
- Antibiotic therapy
- Prompt therapy can improve survival
- Continue for 60 days
- 30-45 days if vaccine administered
48Postexposure Prophylaxis
- Antibiotic therapy
- Same regimen as active treatment
- Substituting oral equivalent for IV
- Ciprofloxacin 500 mg po bid empirically
- Alternatives
- Doxycycline 100 mg po bid
- Amoxicillin 500 mg po tid
49Postexposure Prophylaxis
- Antibiotic therapy
- Children
- Same dose adjustments as treatment
- Weigh benefits vs. risks
- Recommended switch if PCN-susceptible
- Amoxicillin 80 mg/kg/day, max 500 mg tid
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52- Presumptive diagnosis
- History of possible exposure
- Typical signs symptoms
- Rapidly progressing nonspecific illness
- Widened mediastinum on CXR
- Large Gram bacilli from specimens
- Can be seen on Gram stain if hi-grade bacteremia
- Appropriate colonial morphology
- Necrotizing mediastinitis, meningitis at autopsy
53- Definitive diagnosis
- Direct culture on standard blood agar
- Gold standard, widely available
- Alert lab to work up Gram bacilli if found
- 6-24 hours to grow
- Sensitivity depends on severity, prior antibiotic
- Blood, fluid from skin lesions, pleural fluid,
CSF, ascites - Sputum unlikely to be helpful (not a pneumonia)
- Very high specificity if non-motile,
non-hemolytic - Requires biochemical tests for gt99 confirmation
- Available at Reference laboratories
54- Testing for exposure
- Nasal swabs
- Can detect spores prior to illness
- Currently used only as epidemiologic tool
- Decision for PEP based on exposure risk
- May be useful for antibiotic sensitivity in
exposed - Culture on standard media
- Swabs of nares and facial skin
- Serologies
- May be useful from epidemiologic standpoint
55Diagnosis
56Differential Diagnosis
- Inhalational
- Influenza
- Pneumonia
- Community-acquired
- Atypical
- Pneumonic tularemia
- Pneumonic plague
- Mediastinitis
- Bacterial meningitis
- Thoracic aortic aneurysm
- Expect if anthrax
- Flu rapid diagnostic
- More severe in young pts
- No infiltrate
- No prior surgery
- Bloody CSF
- Fever
57Differential Diagnosis
- Cutaneous
- Spider bite
- Ecthyma gangrenosum
- Pyoderma gangrenosum
- Ulceroglandular tularemia
- Mycobacterial ulcer
- Cellulitis
- Expect if anthrax
- fever
- no response to 3º cephs
- painless, black eschar
- /- lymphadenopathy
- usually sig. local edema
58Differential Diagnosis
- Gastrointestinal
- Gastroenteritis
- Typhoid
- Peritonitis
- Perforated ulcer
- Bowel obstruction
- Expect if anthrax
- Critically ill
- Acute abdomen
- Bloody diarrhea
- Fever
59Treatment
- Immediately treat presumptive cases
- Prior to confirmation
- Rapid antibiotics may improve survival
- Differentiate between cases and exposed
- Cases
- Potentially exposed with any signs/symptoms
- Exposed
- Potentially exposed but asymptomatic
- Provide Post-Exposure Prophylaxis
60Treatment
- Hospitalization
- IV antibiotics
- Empiric until sensitivities are known
- Intensive supportive care
- Electrolyte and acid-base imbalances
- Mechanical ventilation
- Hemodynamic support
61Treatment
- Antibiotic selection
- Naturally occurring strains
- Rare penicillin resistance, but inducible
ß-lactamase - Penicillins, aminoglycosides, tetracyclines,
erythromycin, chloramphenicol have been effective - Ciprofloxacin very effective in vitro, animal
studies - Other fluoroquinolones probably effective
- Engineered strains
- Known penicillin, tetracycline resistance
- Highly resistant strains mortality of untreated
62Treatment
- Empiric Therapy
- Adults
- Ciprofloxacin 400 mg IV q12
- OR
- Doxycycline 100mg IV q12
- AND (for inhalational)
- One or two other antibiotics
63Treatment
- Other antibiotic considerations
- Other fluoroquinolones possibly equivalent
- High dose penicillin for 2nd empiric agent
- 50 present with meningitis
- Clindamycin for severe disease
- May reduce toxin production
- Chloramphenicol for known meningitis
- Penetrates blood brain barrier
64Treatment
- Empiric Therapy
- Children
- Ciprofloxacin 10-15 mg/kg/d IV q12, max 1
g/d OR - Doxycycline 2.2 mg/kg IV q12
- (adult dosage if gt8 yo and gt45 kg)
- Add one or two antibiotics for inhalational
- Weigh risks (arthropathy, dental enamel)
65Treatment
- Empiric therapy
- Pregnant women
- Same as other adults
- Weigh small risks (fetal arthropathy) vs benefit
- Immunosuppressed
- same as other adults
66Treatment
- Alternative antibiotics
- If susceptible, or cipro/doxy not possible
- Penicillin, amoxicillin
- Gentamicin, streptomycin
- Erythromycin, chloramphenicol
- Ineffective antibiotics
- Trimethoprim/Sulfamethoxazole
- Third generation cephalosporins
67Treatment
- Antibiotic therapy
- Duration
- 60 days
- Risk of delayed spore germination
- Vaccine availability
- Could reduce to 30-45 days therapy
- Stop antibiotics after 3rd vaccine dose
- Switch to oral
- Clinical improvement
- Patient able to tolerate oral medications
68Treatment
- Other therapies
- Passive immunization
- Anthrax immunoglobulin from horse serum
- Risk of serum sickness
- Antitoxin
- Mutated Protective Antigen
- Blocks cell entry of toxin
- Still immunogenic, could be an alternative
vaccine - Animal models promising
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70Infection Control
- No person to person transmission
- Standard Precautions
- Laboratory safety
- Biosafety Level (BSL) 2 Precautions
71Decontamination
- Highest risk of infection at initial release
- Duration of aerosol viability
- Several hours to one day under optimal conditions
- Covert aerosol long dispersed by recognition 1st
case - Risk of secondary aerosolization is low
- Heavily contaminated small areas
- May benefit from decontamination
- Decontamination may not be feasible for large
areas
72Decontamination
- Skin, clothing
- Thorough washing with soap and water
- Avoid bleach on skin
- Instruments for invasive procedures
- Sterilize, e.g. 5 hypochlorite solution
- Sporicidal agents
- Sodium or calcium hypochlorite (bleach)
73Decontamination
- Suspicious letters/packages
- Do not open or shake
- Place in plastic bag or leakproof container
- If visibly contaminated or container unavailable
- Gently cover paper, clothing, box, trash can
- Leave room/area, isolate room from others
- Thoroughly wash hands with soap and water
- Report to local security / law enforcement
- List all persons in vicinity
74Decontamination
- Opened envelope with suspicious substance
- Gently cover, avoid all contact
- Leave room and isolate from others
- Thoroughly wash hands with soap and water
- Notify local security / law enforcement
- Carefully remove outer clothing, put in plastic
- Shower with soap and water
- List all persons in area
75Outbreak Investigations 2001
- Case definitions
- Confirmed case
- Clinically compatible syndrome
- culture or 2 non-culture diagnostics
- Presumptive case
- Clinically compatible syndrome
- 1 non-culture diagnostic or confirmed exposure
- Exposures
- Confirmed exposure
- May be aided by nasal swab cultures, serology
- Asymptomatic
76Anthrax Essential Notes
- Rapidly fatal flu-like illness in previous
healthy - Widened mediastinum on Chest X-ray
- Painless black skin ulcer
- Non-motile gram positive bacilli in specimens
- Diagnosis primarily by routine culture
- No person-to-person transmission
- Rx prior to prodrome essential for survival
- Empiric therapy ciprofloxacin
- Single inhalational case is an emergency
- Contact Local Health Departments
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83Characteristics of inhalational anthrax cases
among employees of the Washington, D.C.,
Processing and Distribution Center
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