BIODEFENSE

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BIODEFENSE

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Title: BIODEFENSE

1
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BIODEFENSE Epidemiology of Anthrax Shahid
Beheshti University of medical sciences,
2007 By Hatami H. MD. MPH
2
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? ? ??????????? ?????? ? ????(OCCURRENCE)

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2 ???? ?? ????? ?????????

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3
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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

4
Bioweapon 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

5
Bioweapon 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

6
Bioweapon 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

7
Bioweapon Potential

Sverdlovsk, Russia 1979
Accidental release from anthrax drying plant
79 human cases
All downwind of plant
68 deaths
Some infected with multiples strains

8
Bioweapon 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

9
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1 ???? ?????? (Incubation period) 2 ???
?????(Natural course) 3 ??????
?????????(Geographical distribution) 4 ????
?????(Timeline trend) 5 ????? ??? ???? ??? ?
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?????(Predisposing factors) 7 ?????? ?
??????(Susceptibility Resistance) 8 ?????
???? ??? ??????(Secondary attack rate) 9 ????
?????? ? ???? ?????? ????? (Mode of transmission
period of communicability)
10
1 ? ???? ??????

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

11
2 ???? ?? ????? ?????????

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

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

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

14
Pathogenesis

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

15
2 ? ??? ?????

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

16
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?? ????????? ???? ? ??? ??? ?? 60 (?????????)
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17
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??????? 85-1333
18
Anthrax 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
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Bioweapon 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

20
Clinical 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

21
Clinical 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

22
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23
Clinical Features

Cutaneous
Most common areas of exposure
Hands/arms
Neck/head
Incubation period
3-5 days typical
12 days maximum

24
Clinical Features

Cutaneous progression of painless lesions
Papule pruritic
Vesicle/bulla
Ulcer contains organisms, sig. edema
Eschar black, rarely scars

24-36 hrs
days
25
Clinical Features

Cutaneous
Systemic disease may develop
Lymphangitis and lymphadenopathy
If untreated, can progress to sepsis, death

26
Clinical Features

Gastrointestinal
Oropharyngeal
Oral or esophageal ulcer
Regional lymphadenopathy
Edema, ascites
Sepsis
Abdominal
Early symptoms - nausea, vomiting, malaise
Late - hematochezia, acute abdomen, ascites

27
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28
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Occurs worldwide
Endemic areas - Africa, Asia
True incidence not known

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?????? ?? ?(Epidemics)
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31
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All ages and genders affected
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32
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33
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34
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36
Transmission

Human cases historical risk factors
Agricultural
Exposure to livestock
Occupational
Exposure to wool and hides
Woolsorters disease inhalational anthrax
Rarely laboratory-acquired

37
Transmission
38
Transmission

No human-to-human
Naturally occurring cases
Skin exposure
Ingestion
Airborne
Bioterrorism
Aerosol (likely)
Small volume powder (possible)
Foodborne (unlikely)

39
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40
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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

41
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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

Vaccine
Efficacy
gt95 protection vs. aerosol in animal models
gt90 vs. cutaneous in humans

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

45
Postexposure Prophylaxis

Who should receive PEP?
Anyone exposed to anthrax
Empiric antibiotic therapy
Vaccination
Not for contacts of cases, unless also exposed

46
Postexposure 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

47
Postexposure Prophylaxis

Antibiotic therapy
Prompt therapy can improve survival
Continue for 60 days
30-45 days if vaccine administered

48
Postexposure 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

49
Postexposure 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

50
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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

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

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

55
Diagnosis
56
Differential 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

57
Differential 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

58
Differential Diagnosis

Gastrointestinal
Gastroenteritis
Typhoid
Peritonitis
Perforated ulcer
Bowel obstruction

Expect if anthrax
Critically ill
Acute abdomen
Bloody diarrhea
Fever

59
Treatment

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

60
Treatment

Hospitalization
IV antibiotics
Empiric until sensitivities are known
Intensive supportive care
Electrolyte and acid-base imbalances
Mechanical ventilation
Hemodynamic support

61
Treatment

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

62
Treatment

Empiric Therapy
Adults
Ciprofloxacin 400 mg IV q12
OR
Doxycycline 100mg IV q12
AND (for inhalational)
One or two other antibiotics

63
Treatment

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

64
Treatment

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)

65
Treatment

Empiric therapy
Pregnant women
Same as other adults
Weigh small risks (fetal arthropathy) vs benefit
Immunosuppressed
same as other adults

66
Treatment

Alternative antibiotics
If susceptible, or cipro/doxy not possible
Penicillin, amoxicillin
Gentamicin, streptomycin
Erythromycin, chloramphenicol

Ineffective antibiotics
Trimethoprim/Sulfamethoxazole
Third generation cephalosporins

67
Treatment

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

68
Treatment

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

69
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70
Infection Control

No person to person transmission
Standard Precautions
Laboratory safety
Biosafety Level (BSL) 2 Precautions

71
Decontamination

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

72
Decontamination

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)

73
Decontamination

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

74
Decontamination

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

75
Outbreak 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

76
Anthrax 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

77
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79
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80
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81
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(11 ??? 80) ?? 14 ?????? 2001 (23 ???? ??? 1380)
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82
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83
Characteristics of inhalational anthrax cases
among employees of the Washington, D.C.,
Processing and Distribution Center
84
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