PPT – PowerPoint presentation | free to download

About This Presentation

Title:

Description:

Preparing Our Communities Welcome! Faculty Disclosure For Continuing Medical Education (CME) purposes as required by the American Medical Association (AMA) and ... – PowerPoint PPT presentation

Number of Views:63

Avg rating:3.0/5.0

Slides: 77

Provided by: Raym74

Learn more at: https://webmedia.unmc.edu

Category:

Tags: ptosis

more less

Transcript and Presenter's Notes

Title:

1
Preparing Our Communities

Welcome!

2
Faculty Disclosure

For Continuing Medical Education (CME) purposes
as required by the American Medical Association
(AMA) and other continuing education credit
authorizing organizations
In order to assure the highest quality of CME
programming, the AMA requires that faculty
disclose any information relating to a conflict
of interest or potential conflict of interest
prior to the start of an educational activity.
The teaching faculty for the BDLS course offered
today have no relationships / affiliations
relating to a possible conflict of interest to
disclose. Nor will there be any discussion of
off label usage during this course.

3
Biological Events

Chapter 5

3
4
Objectives

Describe the difference between biological events
and bioterrorism (BT)
Discuss public health BT surveillance
Identify the CDC BT Category A agents
Identify emerging infectious diseases
Compare and contrast BT and other CBRNE WMD
utilizing the DISASTER paradigm

4
5
Biological Events

Biological events Natural vs. Intentional

Outbreak of monkey pox in pet prairie
dogs Avian Flu pandemic Natural occurrence of
anthrax Bubonic plague outbreak

5
6
Bioterrorism Release Types Overt or Covert
Covert or Overt ?
Covert or Overt ?
(1763)Captain Simeon Ecuyer had sent
smallpox-infected blankets and handkerchiefs to
the Indians surrounding the fort (as a supposed
peace offering)-- but actually an early example
of biological warfare -- which started an
epidemic among the Indians.
Letter sent to the New York Post and NBC
News Containing white powder
6
7
Potential Methods of Detection
Public Health Surveillance

Increased number of patients
Increased unexplained deaths
Unusual patient age distribution
Unusual seasonality
Unusual manifestation of disease
Animal die-off
Notifiable disease reporting by physicians
other providers
Automated reporting of laboratory results
Number and type of 911 calls
Number and type of EMS runs
Syndromic surveillance

7
8
CDC Categories BT Agents

Divided into Categories A, B,C based on
Quantity of agent available
Ability to disseminate the agent
Person-to-person transmission
Severity of disease
Public response, panic, etc..
Overall risk to national security

8
9
Category A Agents

Anthrax
Smallpox
Plague
Botulinum toxin
Tularemia
Viral hemorrhagic fevers

9
10
Category B Agents(examples)

Infectious Agents
Brucellosis
Glanders

Why are these Category B Agents
Less quantity available than Category A
Harder to disseminate
Less person to person transmission- if any
Slightly less severity of disease
Less known to public - therefore less likely to
cause panic
Slightly less risk to National Security

Bio-toxins
Ricin toxin from Ricinus communis (castor beans)
Staphylococcal enterotoxin B

Water safety threats
Vibrio cholerae
Food safety threats
Salmonella species
Escherichia coli O157H7
Shigella

Viral encephalitis
Venezuelan Equine Encephalitis

10
11
Category C

Emerging infectious diseases as bioterrorism
agents
Nipah virus
Hantavirus
Emerging infectious disease that posses a
significant public health threat
Avian Flu
SARS

11
12

Category A Anthrax

Endemic in animals worldwide with occasional
human cases
Handling infected animal products (especially
cattle, sheep, horses, mules and goats)
Spores used for bioattack
Aerosolized directly or sent in mail/packages
Three forms
Cutaneous, Inhalation, GI

Anthrax in CSFUS index case
12
13
Anthrax Clinical Features

Inhalation
Incubation 2-43 days (may be longer)
Prodrome
Fevers, malaise, dry cough, chest pain, dyspnea,
myalgia
Abrupt onset of fulminant illness
Sudden high fever, respiratory distress, shock
Meningitis in 50
Actual pneumonia uncommon

13
14

Widened mediastinum pleural effusions
Normal Chest X-Ray
Inhalational anthraxUS index case
14
15
Anthrax Clinical Features

Cutaneous
Incubation 1 to 7days (up to 12 days)
Erythematous itchy papule ? ulcer ?
characteristic black eschar with surrounding
erythema and edema
Regional adenopathy and systemic symptoms (e.g.,
fever, malaise)
Most lesions completely resolve

15
16
Anthrax Clinical Features

Gastrointestinal
Incubation period 1-7 days
Not likely after a bioattack
Presents as febrile illness with bloody diarrhea
Eating undercooked infected meat

16
17
Anthrax Diagnosis

Blood cultures
Usually positive in lt 24h
Gram stain pleural fluid or CSF
Sputum gram stain/culture is usually NOT positive
Inhalational disease
Very suggestive if fever and widened mediastinum
Cutaneous disease
Culture fluid from under eschar
Nasal swabs are a poor test

17
18
Anthrax Treatment

Ciprofloxacin 400 mg IV q12h
10-15 mg/kg for children
Other fluoroquinolones probably also effective
OR
Doxycycline 100 mg IV q12h
2.2 mg/kg for children
PLUS
1 or 2 additional antibiotics
Clindamycin, rifampin, vancomycin, penicillin,
chloramphenicol, imipenem, or clarithromycin

18
19
Prophylaxis and Infection Control

Prophylaxis
Ciprofloxacin 500 mg PO BID(Peds10-15 mg/kg)
or
Doxycycline 100 mg PO BID (Peds2.2 mg/kg)
Continue for 60 days (? 100 days)
Vaccine available for DOD forces
Infection Control
Standard barrier precautions are needed
Not transmitted person-to-person
Only immunize / prophylaxis exposed at BT attack

19
20
Anthrax Vaccination Schedule
1
2
3
4
5
6
0
4 weeks
2 weeks
6 months
12 months
18 months

6 shots over 18 months, then annual booster
Dosing schedule is 0.5 mL subcutaneously at each
visit
Then yearly boosters

20
21
Botulism

Clostridium botulinum

A Toxin Producing Obligate, Anaerobic, Spore
Forming, Gram Pos.
Bacillus
21
22
Botulism - General

Caused by a toxin produced by Clostridium
botulinum
Sporadic cases and outbreaks caused by tainted
foods
For bioattack toxin could be delivered as an
aerosol or used to contaminate food / water

22
23
Botulism - Clinical Features

12 to 36 hour incubation
Range 2 h to 8 days
Clinical recognition is key to diagnosis
Bulbar palsies Must be present!
Ptosis, blurred vision, dry mouth, dysarthria,
trouble swallowing
Afebrile,AAO x 3, difficulty speaking
Descending skeletal muscle paralysis
Death Respiratory muscle paralysis

23
24
17 Year-Old with Mild Botulism
24
25
Botulism - Treatment

Supportive care
Respiratory failure
Prolonged Ventilator support
Antitoxin
State health department obtained
Prevents further damage
Does not alter current damage

25
26
Botulism Infection Control

Prophylaxis
No proven prophylaxis at this time
Investigational Vaccine
Isolation
Standard precautions (not P-to-P)
Need to contact public health authority
immediately Others may be exposed to
contaminated food source or agent

26
27
Plague
Yersinia pestis

Yersinia pestis

Source www.cdc.gov
Gram Neg., Anaerobic, Rod Shaped Bac. Safety
Pin Bipolar on Wright Staining
27
28
Plague - General

Endemic in animals throughout the world
Prairie dogs in the Southwestern US
High potential as a BT agent
Endemic form
Spread to humans via a flea vector
Results in bubonic form of the disease
Bioattack
Most likely aerosolized
Results in pneumonic plague
Release of infected fleas

Buboes
Source www.cdc.gov
28
29
Plague Clinical Features

Following Aerosolized Bioattack
1- 6 day incubation
Abrupt onset
High fever, chills, and malaise
Cough with bloody sputum
Sepsis
Severe rapidly progressive pneumonia
Untreated 100 mortality

29
30
Plague - Diagnosis

CXR with patchy infiltrates
Culture of blood and sputum
Need to inform the laboratory if you suspect
plague special techniques
May show characteristic safety-pin bipolar
staining
Sudden Gm(neg) pneumonia

30
31
Plague pneumonia
Normal Chest X-Ray
31
32
Plague - Treatment

Preferred Start within first 24 hours for 10
days
Streptomycin 1 g IM q12h
15 mg/kg/dose for children
Avoid in pregnant women
Gentamicin 5 mg /kg IM or IV qd
Or 2 mg/kg load the 1.7 mg/kg q8h
For children use 2.5 mg/kg q8h
Alternative
Doxycycline 100 mg IV q12h
2.2 mg/kg/dose q12h for children
Ciprofloxacin 400 mg IV q12h
Other fluoroquinolones probably effective
For children 15 mg/kg/dose q12h

32
33
Plague - Infection Control

Prophylaxis Treat for 7 days
Doxycycline 100 mg PO bid
2.2 mg/kg for children
Ciprofloxacin 500 mg PO bid
20 mg/kg for children
other fluoroquinolones probably effective
Isolation
Droplet precautions (Yes, P-to-P)

33
34
Smallpox

Source www.cdc.gov
34
35
Smallpox - General

One of the deadliest disease
Mortality rate of 30
US stopped vaccinating in 1972
Declared eradicated by WHO
In 1980, however...
Bioattack
Aerosolized virus or by exposure to purposefully
infected terrorists

35
36
Smallpox - Clinical Features

Incubation period
7-17 day (average 12d), Weaponized 3-5 d
Severe prodrome Key difference!
2-3 day of fever, severe myalgias, prostration,
occ. n/v, delerium
10 with light facial erythematous rash
Distinctive rash
Initially on face and extremities
Including palms and soles
Spreads to trunk

36
37
Small Pox - Clinical Features

Rash
Macules ? papules ? vesicles ? pustules
Unlike chicken pox, lesions dont appear in
crops
All lesions in an area are in the same stage of
development
Lesions are firm, deep, frequently umbilicated
Rash scabs over in 1-2 weeks

Chickenpox
Smallpox
37
Source www.cdc.gov
38
Smallpox
The main diagnostic tool for smallpox
Source www.cdc.gov
is the history and physical!
38
39
Smallpox - Treatment

Vaccination
In the early stages of disease
Supportive care
Penicillinase-resistant antibiotics (for
secondary infection)
Daily eye rinsing
Adequate hydration and nutrition
FDA has not approved specific therapy
Topical idoxuridine for corneal lesions (Dendrid)
Cidofovir ?

39
40
Smallpox - Infection Control

Prophylaxis
Vaccine is effective if given within 3 days of
exposure
Isolation
Airborne and contact precautions
Febrile illness after potential exposure should
prompt isolation before rash starts
Immediate contact your hospital epidemiologist
and the public health authorities

40
41
Tularemia

Francisella tularensis

Source www.cdc.gov
Gram Neg. Coccobacillus
41
42
Tularemia - General

Endemic in North America and Eurasia
Sporadic human cases spread by ticks or biting
flies
Occasionally from direct contact with infected
animals (ulceroglandular)
Bioattack
Aerosolized bacteria
Typhoidal tularemia ( / - ) pneumonia

42
43
Tularemia - Clinical Features

Bioattack
3-5 day incubation (range 1-14 days)
Acute febrile illness with prostration
80 will have radiographic evidence of pneumonia
May have associated conjunctivitis or skin ulcer
regional adenopathy

43
44
Tularemia - Diagnosis

Culture of blood and sputum
May take weeks to isolate and ID
Gram negative coccobacillus
Confirmation may require reference laboratory
Potential hazard to laboratory personnel
Laboratory must be notified if tularemia is
suspected

44
45
Tularemia - Treatment

Preferred Treatment time varies with Abx
Streptomycin 1 g IM q12h
15 mg/kg for children
Gentamicin 5 mg / kg IM or IB q day
for children use 2.5 mg/kg q8h
Alternative
Doxycycline 100 mg IV q12h
2.2 mg/kg for children
Ciprofloxacin 400 mg IV q12h
Children 15 mg/kg
Other fluoroquinolones probably effective

45
46
Tularemia - Infection Control

Prophylaxis Treat for 14 days
Doxycycline 100 mg PO bid
2.2 mg/kg for children
Ciprofloxacin 500 mg PO bid
15-20 mg/kg for children
Tetracycline
Isolation
Standard precautions (Not P-to-P)

46
47
Viral Hemorrhagic Fevers
Source www.cdc.gov
Ebola virus
47
48
VHF - General

Naturally occurring disease
Transmitted to humans by contact with infected
animals or arthropod vectors.
Sporadic outbreaks in Africa, parts of Asia and
Europe (Outside of Africa, likely BT event)
VHF viruses as bioterrorism agents
Weaponized by several countries
Aerosolization
Case fatality rates
Omsk hemorrhagic fever 0.5
Ebola 90

48
49
VHF - Clinical Features

Incubation 2 - 21days
Depends on virus
Initial presentation
Nonspecific prodrome (fever, myalgias, headache,
abdominal pain, prostration)
Exam may show only flushing of face and chest,
conjunctival injection, and petechiae
Disease progresses to generalized mucous membrane
hemorrhage and shock occurs

Marburg Disease
Bolivian Hemorrhagic Fever
49
50
VHF - Diagnosis

Ancillary testing
Thrombocytopenia, leukopenia, AST elevation
common
Definitive diagnosis requires detection of
antigens or antibodies
Testing done at CDC
Do not wait to confirm the diagnosis before
notifying the local public health authorities

50
51
VHF - Treatment

Supportive care
Ribavirin may be useful
Best early in the course of illness
Adults and children 30 mg/kg IV load (max 2
g)
then 16 mg/kg (max 1g) q6h x 4 days
then 8 mg/kg (max 500 mg) IV q8h for 6 days
Oral dosing regimen is available

51
52
VHF - Infection Control

Prophylaxis
None at this time
Vaccine in primates being tested
Isolation Key!
Blood and bodily fluids extremely infectious
Liquid-impervious protective coverings, including
leg and shoe coverings
Double gloves, Face shields or goggles
N-95 or better respirators
Negative pressure room

52
53
Emerging Infectious Diseases

53
54
Pandemic
A Global Epidemic!
54
55
Past flu pandemics
1918 Spanish Flu
1957 Asian Flu
1968 Hong Kong Flu
A(H1N1)
A(H2N2)
A(H3N2)
20-40 m deaths 675,000 US deaths
1-4 m deaths 70,000 US deaths
1-4 m deaths 34,000 US deaths
55
56
Put another way
56
57
Pandemic Influenzawww.cdc.gov
57
58
Pandemic Influenza
58
59
Pandemic Influenza Healthcare Workforce

Who is going to show up for work?
The reports, articles and plans are alarming!
Will you?

59
60
Containment

Limit travel
Isolate ill and quarantine exposed
Trace contacts
Curfews cancel public gatherings
Prophylaxis treatment
Neuramidase inhibitors ?
Vaccine ?

60
61

D Detection
I Incident Command
S Safety Security
A Assess Hazards
S Support
T Triage Treatment
E Evacuation
R Recovery

61
62

Detection

There may not be a scene May be hard to
detect Long Incubation period Symptoms manifest
slowly Non-specific symptoms
Beware of multiple people with similar Complaints,
particularly in the healthy population
62
63