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BIODEFENCE

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Lives in dry sputum, corpses, flea feces. Inactivated by sunlight in a few hours ... Flea-bite (most common) Handling infected animals- skin contact, scratch, bite ... – PowerPoint PPT presentation

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Title: BIODEFENCE


1
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BIODEFENCE Epidemiology of Plague Shahid Beheshti
University of medical sciences, 2005 By Hatami
H. MD. MPH
2
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? ? ??????????? ?????? ? ????(OCCURRENCE)
  • 1- ????? ? ????? ???????
  • 2 ???? ?? ????? ?????????

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3
1- Definition
  • A special zoonosis involving rodents and their
    fleas
  • Transmits to various animals and to human

4
Importance
  • One of three WHO quarantinable diseases
  • Estimated 200 million deaths recorded
  • Three prior pandemics
  • Justinian 541 AD
  • Black Death 1346
  • China 1855

5
Importance
  • 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

6
Bioweapon 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

7
Bioweapon Potential
  • Estimated Effect
  • Aerosol release 50kg Y. pestis over city of 5
    million people
  • 150,000 infected
  • 36,000 die

8
Bioweapon Potential
  • Delivery Mechanism
  • Aerosol
  • Bioweapons programs developed techniques to
    aerosolize plague directly
  • Pneumonic form would be expected
  • Proven infectivity of primates

9
Factors 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

10
Factors suggesting BT aerosol
  • Epidemic of severe/fatal pneumonia (hemoptysis)
  • Symptoms 1-6 days after exposure
  • Occurs in persons without risk factors

11
2- Etiologic agent
  • Taxonomy
  • Family Enterobacteriaceae
  • 11 Yersinia species 3 human
    pathogens
  • Y. pestis
  • Y. pseudotuberculosis
  • Y. enterocolitica

12
Microbiology
  • Staining
  • Gram negative coccobacillus
  • Giemsa, Wright, Wayson stains bipolar staining

13
Environmental 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

14
Pathogenesis
  • 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

15
Pathogenesis
  • Intracellular organism
  • Survives in monocytes/macrophages
  • Inhalation (pneumonic form)
  • Deposition into alveoli
  • Classic lobular pneumonia
  • Resulting manifestation
  • liquefaction necrosis, residual scarring

16
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1 ???? ?????? (Incubation period) 2 ???
?????(Natural course) 3 ??????
?????????(Geographical distribution) 4 ????
?????(Timeline trend) 5 ????? ??? ???? ??? ?
?????? ??????? 6 ????? ????? ?????
?????(Predisposing factors) 7 ?????? ?
??????(Susceptibility Resistance) 8 ?????
???? ??? ??????(Secondary attack rate) 9 ????
?????? ? ???? ?????? ????? (Mode of transmission
period of communicability)
17
1 ? ???? ??????
  • Incubation Period
  • 1-7 days
  • Longer in immunized individuals
  • For primary pneumonia, 1-4 days
  • Ref. Control of communicable diseases

18
Clinical Features
2 ? ??? ?????
  • Three types of Disease
  • Bubonic
  • Septicemic
  • Pneumonic

19
Clinical Features
  • Bubonic
  • Classic
  • Predominates )84(
  • Usually from bite of infectious flea
  • Contact ingestion of infected animals

20
Clinical Features
  • Buboes
  • Enlarged tender lymph nodes
  • Usually unilateral
  • Usually inguinal/femoral in adults
  • Cervical/submaxillary more common in age lt 10

Image Armstrong Cohen
21
Clinical 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

22
Clinical Features
  • Septicemic
  • Historically 12
  • Secondary
  • if complication of bubonic
  • Primary
  • if no buboes detected

23
Clinical Features
  • Septicemic
  • Similar to other gram-negative sepsis
  • Mortality
  • Overall 50
  • gt 90 untreated
  • Usually from late diagnosis and Rx

24
Clinical Features
  • Pnuemonic
  • Approx. 2 all plague are primary pneumonic
  • Secondary
  • if preceding bubonic (most cases) or septicemic

25
Clinical 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

26
Clinical 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.

27
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28
Clinical 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

29
Clinical 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

30
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31
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32
Geographic 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

33
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34
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35
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36
4 ? ???? ?????
  • ?????? ?? ?(Pandemics)
  • ?????? ?? ?(Epidemics)
  • ????? ?? ? (Outbreaks)
  • ????? ????? ? (Duration)
  • ????? ???? ?(Seasonality)

37
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38
6 ? ????? ????? ????? ?????
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39
Risk 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

40
7 ? ?????? ? ?????? ?? ????? ??????
  • ?????? ?????
  • ?????? ??????? ??? ?? ??????
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41
8 ? ????? ????? ??????
  • Pneumonic plague may be highly communicable under
    appropriate climatic conditions

42
9 ? ????? ? ????? ? ???? ?????? ?????? ? ????
?????? ????? ?????
43
Transmission
  • 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

44
Transmission
Bioterrorism
45
Period of communicability
  • Duration of isolation
  • 2 days after initiating antibiotics and
    clinically improved
  • After sputum cultures negative

46
Reservoir
  • Wild rodents
  • Rabies hares
  • Wild carnivores
  • Domestic cats

47
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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

48
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1 ? ?????? ????????? ??????? ???? 2 ? ??? ??????
?????? (????? ????? ????? ?????? . . . 3 ?
?????????? ?? ???????? (????? ???????) ?
?????????????
49
Prevention
  • 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

50
Prevention
  • 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

51
Infection 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

52
Infection 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

53
Infection 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

54
Infection Control
  • Corpses
  • Standard strict precautions by trained personnel
  • Transport same as live patient
  • Avoid aerosolizing procedures or use HEPA filters
    and negative pressure room

55
Infection 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

56
Infection Control
  • National control programs
  • Surveillance
  • Early diagnosis, treatment isolation of cases
  • Environmental sanitation exposure avoidance
  • Public education

57
Decontamination
  • 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

58
Decontamination
  • Patient rooms
  • Usual cleaning
  • Use standard precautions
  • Disinfect contaminated linens
  • Standard disinfectants

59
Post-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

60
Post-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

61
Post-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

62
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1 ? ????? ????? 2 ? ????? ?? ???? 3 ? ???? ??
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63
Diagnosis
  • 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

64
Diagnosis
  • 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

65
Treatment
  • Start immediately upon suspicion of diagnosis
  • Delay gt1day after symptoms usually fatal

66
Treatment
  • 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

67
Treatment
  • 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

68
Treatment
  • 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)

69
Treatment
  • 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

70
Treatment
  • 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)

71
Treatment
  • 2nd choices
  • Alternatives sulfonamides
  • If other antibiotics not available
  • Ineffective for pneumonic
  • TMP-SMX
  • Generally ineffective
  • ?-lactams, rifampin, aztreonam, macrolides

72
Treatment
  • Antibiotic resistance rare
  • May be expected in BT scenario (engineered
    agents)

73
Treatment
  • 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

74
Treatment
  • Bubo care
  • Usually recedes with antibiotics
  • Rarely become fluctuant/abscessed
  • Unnecessary I D increases contacts risks

75
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76
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77
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78
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