Title: BIODEFENCE
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BIODEFENCE Epidemiology of Plague Shahid Beheshti
University of medical sciences, 2005 By Hatami
H. MD. MPH
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31- Definition
- A special zoonosis involving rodents and their
fleas - Transmits to various animals and to human
4Importance
- One of three WHO quarantinable diseases
- Estimated 200 million deaths recorded
- Three prior pandemics
- Justinian 541 AD
- Black Death 1346
- China 1855
5Importance
- Naturally occurring human outbreaks parallel and
follow epizootics - BT event may also spawn sylvatic plague
- Following disasters
- Disruption of rat habitats
- Transport of disease
- through rat relocation
6Bioweapon Potential
- One of top 6 agents identified by CDC (category
A) - Known attempted uses
- In kaffa
- Japanese (Unit 731) WWII infected fleas released
over China - Weapons programs
- U.S. terminated 1970
- Russia unknown
7Bioweapon Potential
- Estimated Effect
- Aerosol release 50kg Y. pestis over city of 5
million people - 150,000 infected
- 36,000 die
8Bioweapon Potential
- Delivery Mechanism
- Aerosol
- Bioweapons programs developed techniques to
aerosolize plague directly - Pneumonic form would be expected
- Proven infectivity of primates
9Factors suggesting BT aerosol
- Several cases of primary pneumonic (no or few
bubonic) - Peak in number of previously healthy persons with
cough, fever, death - Many with GI symptoms
- Occurs in non-endemic area
10Factors suggesting BT aerosol
- Epidemic of severe/fatal pneumonia (hemoptysis)
- Symptoms 1-6 days after exposure
- Occurs in persons without risk factors
112- Etiologic agent
- Taxonomy
- Family Enterobacteriaceae
- 11 Yersinia species 3 human
pathogens - Y. pestis
- Y. pseudotuberculosis
- Y. enterocolitica
12Microbiology
- Staining
- Gram negative coccobacillus
- Giemsa, Wright, Wayson stains bipolar staining
13Environmental Survival
- Requires host
- Does not survive in environment well
- Can live weeks in water, moist soil
- Lives months/years at just above freezing
temperature - Lives only 15 minutes in 55 C
- Lives in dry sputum, corpses, flea feces
- Inactivated by sunlight in a few hours
14Pathogenesis
- Highly virulent and invasive
- Four routes human disease
- Flea-bite (most common)
- Handling infected animals- skin contact, scratch,
bite - Inhalation from humans or animals
- Ingesting infected meat
15Pathogenesis
- Intracellular organism
- Survives in monocytes/macrophages
- Inhalation (pneumonic form)
- Deposition into alveoli
- Classic lobular pneumonia
- Resulting manifestation
- liquefaction necrosis, residual scarring
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period of communicability)
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- Incubation Period
- 1-7 days
- Longer in immunized individuals
- For primary pneumonia, 1-4 days
- Ref. Control of communicable diseases
18Clinical Features
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- Three types of Disease
- Bubonic
- Septicemic
- Pneumonic
19Clinical Features
- Bubonic
- Classic
- Predominates )84(
- Usually from bite of infectious flea
- Contact ingestion of infected animals
20Clinical Features
- Buboes
- Enlarged tender lymph nodes
- Usually unilateral
- Usually inguinal/femoral in adults
- Cervical/submaxillary more common in age lt 10
Image Armstrong Cohen
21Clinical Features
- Bubonic
- Mortality
- 40-60 untreated, lt5 treated
- Overall case fatality 14 in U.S.
- Usually from delayed Dx and Rx
- Complications
- Often develop bacteremia
- Some develop
- Septicemia (secondary septicemic plague)
- Pneumonic (secondary pneumonic plague)
- meningitis
22Clinical Features
- Septicemic
- Historically 12
- Secondary
- if complication of bubonic
- Primary
- if no buboes detected
23Clinical Features
- Septicemic
- Similar to other gram-negative sepsis
- Mortality
- Overall 50
- gt 90 untreated
- Usually from late diagnosis and Rx
24Clinical Features
- Pnuemonic
- Approx. 2 all plague are primary pneumonic
- Secondary
- if preceding bubonic (most cases) or septicemic
25Clinical Features
- Pneumonic
- Primary if result of droplet inhalation
- From other pneumonic plague patients or infected
animals - From expected if aerosolized as a bioweapon
- Extremely infectious via droplets and purulent
sputum
26Clinical Features
- Pneumonic
- Mortality
- Nearly 100 untreated or if delayed gt 24 hrs
after symptom onset - High despite treatment
- Overall case fatality 57 in U.S.
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28Clinical Features
- In BT event pneumonic form most likely
- Pneumonic
- incubation 1-6 days for primary
- Initialacute flu-like , myalgia, malaise
- Often prominent GI , abd pain
- Severe pneumonia
- Within 24hr of onset
- Cough, hemoptysis
- Progresses to cyanosis, stridor
- Death usually occurs 2-4 days after exposure
29Clinical Features
- Immunity
- Several days after infection
- lt5 never
- Transient, not life-long immunity after surviving
- May not protect against a large inoculum
- Antibody levels normalize in months-years
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32Geographic distribution
- Globally
- Approximately 1500 cases/year since 1965
- 25 countries reported cases
- gt 50 Eastern, S. Africa,
- U.S.
- 390 cases/year reported 1947-96
- Southwest region of U.S. endemic
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- ????? ?? ? (Outbreaks)
- ????? ????? ? (Duration)
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39Risk factors
- Close contact with case
- Contact with infected animal
- Living or recent travel in endemic area
- Residing in crowded conditions
- Cool, wet weather
- Exposure to a known intentional release
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- Pneumonic plague may be highly communicable under
appropriate climatic conditions
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43Transmission
- Mostly endemic sylvatic plague with sporadic
cases - Person to person spread
- Higher risk in
- Overcrowding,
- Indoor contacts,
- Cold/wet weather
- Fleas may remain infective for months
44Transmission
Bioterrorism
45Period of communicability
- Duration of isolation
- 2 days after initiating antibiotics and
clinically improved - After sputum cultures negative
46Reservoir
- Wild rodents
- Rabies hares
- Wild carnivores
- Domestic cats
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- 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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49Prevention
- Vaccination
- - Bubonic only
- Killed virulent strain
- No longer commercially available
- Series
- 3 primary (0 , 3 mo and 6 mo later)
- boosters at 6 mo intervals
50Prevention
- Vaccination
- Indications
- Lab workers
- Military personnel stationed in endemic areas
- Efficacy
- Based on WWII (0 cases) and Vietnam (3 cases)
troops - Protects vs. bubonic only, not pneumonic
51Infection Control
- Respiratory Droplet Precautions
- Wear mask, gown, gloves, eye protection
- Suspected cases - isolate
- Immediately respiratory (even for bubonic)
- Avoid unnecessary close contact 1st 48 hrs of abx
- Duration
- 2 days after initiating antibiotics and
clinically improved - After sputum cultures negative
52Infection Control
- Respiratory Droplet Precautions
- Mask during transport
- Can cohort if not enough room
- Contacts consider isolation
- Recommended for those receiving PEP
- During 1st 48 hrs of Rx
- Not recommended for those refusing PEP
- but still observe 7 days
53Infection Control
- Standard Precautions
- Successfully treated cases after 48hr of abx
- Laboratory safety
- Alert lab if suspected
- BSL-2 for normal procedures
- BSL-3 if hi risk aerosolizing or resistant
strains
54Infection Control
- Corpses
- Standard strict precautions by trained personnel
- Transport same as live patient
- Avoid aerosolizing procedures or use HEPA filters
and negative pressure room
55Infection Control
- Outbreak measures
- Establish source
- Define geographical boundaries
- Establish active surveillance
- Laboratory confirmation of cases
- Isolation of pneumonic cases
- Rapid treatment of cases and contacts
- Flea and rodent control
56Infection Control
- National control programs
- Surveillance
- Early diagnosis, treatment isolation of cases
- Environmental sanitation exposure avoidance
- Public education
57Decontamination
- Environment
- Aerosol dispersed within an hour fragile
- No evidence residual bacteria are a threat
- No environmental decon. indicated
- May need surveillance measures for rodents/fleas
in area
58Decontamination
- Patient rooms
- Usual cleaning
- Use standard precautions
- Disinfect contaminated linens
- Standard disinfectants
59Post-exposure Prophylaxis
- Also for mass causalities
- For all asymptomatic contacts of suspected
untreated pneumonic cases - Contact within last 6 days
- Untreated pneumonic lt48hr approp treatment
- Those within 2 meters of case
- Household, hospital contacts
- Those who might have been exposed to initial
aerosol - Seek out homeless, mental handicaps, homebound
60Post-exposure Prophylaxis
- Antibiotics
- 1st choices
- Tetracyclines
- Doxycycline
- 100 po bid adults and kids gt45 kg
- 2.2 mg/kg po bid for kids lt45 kg
- Tetracycline equivalent dosages
- Fluoroquinolones
- Ciprofloxacin
- 500 mg po bid for adults
- 20 mg/kg po bid (max 1g/day) for kids
- Others at equivalent dosages
61Post-exposure Prophylaxis
- Alternatives
- Chloramphenical 25 mg/kg po qid
- Not in kids lt2yo
- For pregnant breastfeeding women
- Same as adults above but no tetracycline
- Doxycycline may be used
- Duration
- 7 days since last exposure PEP
- 10 days for mass casualties
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63Diagnosis
- No rapid tests available treat first
- Report suspected cases to local health dept if no
risk factor for naturally occurring disease - Send out samples if not done in hospital
- Obtain specimens as indicated
- Blood attempt 4 samples q30 min
- Bubo aspirate (inject 1-2cc saline and aspirate
with 20 Ga needle) - Sputum
- CSF
64Diagnosis
- CXR
- Inoculate on/in infusion broth, blood agar,
McConkey agar - Biochemical profiles if automated system has
capacity to detect - Stains Gram and Waysons or Giemsa
- DFA testing
- Acute serum for F1 antibody
- CDC sample for bacteriophage lysis
65Treatment
- Start immediately upon suspicion of diagnosis
- Delay gt1day after symptoms usually fatal
66Treatment
- Antibiotics
- General
- Contained casualties IV
- Mass casualties po equivalent, same as
post-exposure prophylaxis - Also need intensive supportive care
- Ventilation
- Pressors usually not needed
- Who to treat
- Suspected cases
- Index
- If suspected release anyone with fever, cough
67Treatment
- Special populations
- Children
- Same as adults but try avoid TCN if lt8yo
- No chloramphenicol for lt2 yo (grey baby syndrome)
- Pregnant women
- Try to avoid streptomycin
- 1st choice gentamicin, same adult dose
- 2nd choice doxy, same adult dose
- 3rd choice cipro, same adult dose
- Breastfeeding women
- Same recommendations as pregnant
- Immunosuppressed no different than competent
68Treatment
- Antibiotics for contained casualties
- (For mass casualties, same as PEP)
- 1st choices
- Streptomycin - FDA-approved
- 30 mg/kg IM divided q8-12 kids (max 2g/day)
- 1g IM bid adult
- bacteriocidal
- gentamicin as effective, more avail, qd dosing
- 5mg/kg iv qd, w/levels or load 2mg/kg then
1.7mg/kg q8 - 2.5mg/kg im/iv q8h kids (q12hr for lt1wk or
premature)
69Treatment
- 2nd choices
- tetracyclines - as good in vitro, good human data
- doxycycline
- single 200mg iv loading dose (some sources)
- 100mg iv bid or 200 mg iv qd adults kids gt45kg
- 2.2mg/kg iv q12hr (max 200mg) kids lt45kg
- Better absorption, distribution, half-life than
TCN - 1st choice po therapy for mass casualties
- tetracycline
- 500 mg po qid adults
- 6.25-12.5 mg/kg po qid kids gt9yo
70Treatment
- 2nd choices
- Fluoroquinolonesbetter in vitro, no human data
- ciprofloxacin
- 400 mg iv q12hr adults
- 15 mg/kg iv q12hr kids (max 1g/day)
- Levofloxacin
- Ofloxacin
- Chloramphenicol
- 1st choice for meningitis /- aminoglycoside
- Crosses blood-brain barrier
- 25mg/kg iv q6hr adults kids, keep level 5-20
µg/ml - Avoid in kids lt2 yo (grey baby syndrome)
71Treatment
- 2nd choices
- Alternatives sulfonamides
- If other antibiotics not available
- Ineffective for pneumonic
- TMP-SMX
- Generally ineffective
- ?-lactams, rifampin, aztreonam, macrolides
72Treatment
- Antibiotic resistance rare
- May be expected in BT scenario (engineered
agents)
73Treatment
- Switch to po when improved, tolerates
- Usual response
- Bubonic improved in 2-3d, afebrile 2-5d
- Duration 10-14 days or 3 days after afebrile,
improving - Supportive care
- Volume status maintenance
- Hemodynamic monitoring
- pressors not usually needed
- Support of multiorgan failure
74Treatment
- Bubo care
- Usually recedes with antibiotics
- Rarely become fluctuant/abscessed
- Unnecessary I D increases contacts risks
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