Dog Bite
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39 slides
Jul 17, 2009
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Dog Bites
Dogs
•Prominent canine teeth
•Enormous pressure when biting
•Large breeds tend to cause
wounds in the head and neck
•Powerful jaws can penetrate the skull and
destroy deep tissue
•Prominent canine teeth
•Enormous pressure when biting
•Large breeds tend to cause
wounds in the head and neck
•Powerful jaws can penetrate the skull and
destroy deep tissue
Victims
•Males are more likely to be bitten by dogs.
•Females are more likely to be bitten by
cats.
•Animal bites are most common in children
aged 5-14 years
•Males are more likely to be bitten by dogs.
•Females are more likely to be bitten by
cats.
•Animal bites are most common in children
aged 5-14 years
Cause
•Causes of provoked attacks
–Antagonizing an animal
–Hurting an animal
•Causes of unprovoked attacks
–Approaching the young of an animal
–Approaching an animal that is eating
–Entering the property of a territorial animal
–Nearing an animal with rabies
•Causes of provoked attacks
–Antagonizing an animal
–Hurting an animal
•Causes of unprovoked attacks
–Approaching the young of an animal
–Approaching an animal that is eating
–Entering the property of a territorial animal
–Nearing an animal with rabies
Mortality/Morbidity
•Wound infection and cellulitis
–Puncture wounds have a higher rate
of infection than lacerations
–Lacerations cause more damage to tissues
than puncture wounds
–Septic arthritis from wounds in joint spaces
•Osteomyelitis from deep wounds
•Meningitis from penetrating skull wounds
•Rabies
•Wound infection and cellulitis
–Puncture wounds have a higher rate
of infection than lacerations
–Lacerations cause more damage to tissues
than puncture wounds
–Septic arthritis from wounds in joint spaces
•Osteomyelitis from deep wounds
•Meningitis from penetrating skull wounds
•Rabies
Exams and Tests
•Inspection the wound
•X-rays to look for fractures or foreign body
in the wound.
•Inspection the wound
•X-rays to look for fractures or foreign body
in the wound.
Rabies contacted Category
Category Contact
Category I
touching or feeding suspect animals,
but skin is intact
Category II
minor scratches without bleeding
from contact, or licks on broken skin
Category III
one or more bites, scratches, licks
on
broken skin, or other contact that
breaks the skin; or exposure to bats
Category Contact
Category I
touching or feeding suspect animals,
but skin is intact
Category II
minor scratches without bleeding
from contact, or licks on broken skin
Category III
one or more bites, scratches, licks
on
broken skin, or other contact that
breaks the skin; or exposure to bats
Treatment
•Wound care
–Irrigation and Debridement
•Suture:
–Primary closure in facial wounds
( rarely infected because of well vascularized)
–Delayed closure
•heavily contaminated (dirty)
•significant amount of tissue damage
•hands or lower extremities or
•wound older than 6 hours
–Some wounds are never sutured
•Wound care
–Irrigation and Debridement
•Suture:
–Primary closure in facial wounds
( rarely infected because of well vascularized)
–Delayed closure
•heavily contaminated (dirty)
•significant amount of tissue damage
•hands or lower extremities or
•wound older than 6 hours
–Some wounds are never sutured
Medical treatment
•Antibiotic coverage for
–staphylococci
–anaerobes
•Tetanus prophylaxis
•Rabies prophylaxis
•Antibiotic coverage for
–staphylococci
–anaerobes
•Tetanus prophylaxis
•Rabies prophylaxis
Antibiotics commonly used
•Amoxicillin clavulanate (Augmentin
®
)
•Ampicillin-sulbactam (Unasyn
®
)
•Trimethoprim and sulfamethoxazole (Bactrim
®
)
•Clindamycin (Cleocin
®
)
•Erythromycin (E-Mycin, Ery-Tab, Erythrocin)
•Ceftriaxone (Rocephin
®
)
•Tetracycline (Sumycin
®
)
•Amoxicillin clavulanate (Augmentin
®
)
•Ampicillin-sulbactam (Unasyn
®
)
•Trimethoprim and sulfamethoxazole (Bactrim
®
)
•Clindamycin (Cleocin
®
)
•Erythromycin (E-Mycin, Ery-Tab, Erythrocin)
•Ceftriaxone (Rocephin
®
)
•Tetracycline (Sumycin
®
)
Vaccines and immune globulins
•Tetanus toxoid
•Rabies vaccine
•Rabies immune globulin
•Tetanus toxoid
•Rabies vaccine
•Rabies immune globulin
Tetanus vaccine
Dose 1 Dose 2 Dose 3
Day 0 Month 1-2Month 6-12
Intramuscular injection
Dose 1 Dose 2 Dose 3
Day 0 Month 1-2Month 6-12
Intramuscular injection
Tetanus prophylaxis consideration
IMMUNIZATION HISTORY
CLEAN
MINOR
WOUND
ALL OTHER
WOUNDS
1. Fewer than 3 doses; or
2. Uncertain number of doses; or
3. No immunization
TT only
TT +
TIG*
At least 3 previous doses of tetanus vaccine,
but the most recent more than 10 years ago
TT only TT only
At least 3 previous doses of tetanus vaccine,
but the most recent more than 5 and less than
10 years ago
no
immunization
required
TT only
At least 3 doses of tetanus, with the most
recent 5 years ago or less
no
immunization
required
no
immunization
required
http://www.health.gov.nl.ca/health/publications/immunization/S5/tetanus_prophylaxis_in_wound_man.htm
TIG*= Tetanus Immune Globolin
IMMUNIZATION HISTORY
CLEAN
MINOR
WOUND
ALL OTHER
WOUNDS
1. Fewer than 3 doses; or
2. Uncertain number of doses; or
3. No immunization
TT only
TT +
TIG*
At least 3 previous doses of tetanus vaccine,
but the most recent more than 10 years ago
TT only TT only
At least 3 previous doses of tetanus vaccine,
but the most recent more than 5 and less than
10 years ago
no
immunization
required
TT only
At least 3 doses of tetanus, with the most
recent 5 years ago or less
no
immunization
required
no
immunization
required
http://www.health.gov.nl.ca/health/publications/immunization/S5/tetanus_prophylaxis_in_wound_man.htm
TIG*= Tetanus Immune Globolin
Rabies vaccine
•Protection level should be achieved by day 14 of
a post-exposure immunization regimen, with or
without simultaneous administration of RIG and
irrespective of age.
•Protection level should be achieved by day 14 of
a post-exposure immunization regimen, with or
without simultaneous administration of RIG and
irrespective of age.
Vaccine & RIG consideration
Category Contact Immunization
Category I
touching or feeding suspect animals,
but skin is intact
None
Category II
minor scratches without bleeding
from contact, or licks on broken skin
Vaccine
Category III
one or more bites, scratches, licks on
broken skin, or other contact that
breaks the skin; or exposure to bats
Vaccine + RIG
Category Contact Immunization
Category I
touching or feeding suspect animals,
but skin is intact
None
Category II
minor scratches without bleeding
from contact, or licks on broken skin
Vaccine
Category III
one or more bites, scratches, licks on
broken skin, or other contact that
breaks the skin; or exposure to bats
Vaccine + RIG
Post-exposure rabies vaccination
schedule
Day
Regimen
dose0 3 7143090
5 dose IM 0.51 1 1 1 1
4 dose IM 0.52 0 1 0
1
(21)
8 site ID 0.18 0 4 0 1 1
2 site ID 0.12 2 2 0 1 1
schedule
Day
Regimen
dose0 3 7143090
5 dose IM 0.51 1 1 1 1
4 dose IM 0.52 0 1 0
1
(21)
8 site ID 0.18 0 4 0 1 1
2 site ID 0.12 2 2 0 1 1
07/17/09 17
8 sites Intradermal administration
Day 0
Day 0
Day 07
Day 07
30Day 0790
8 sites Intradermal administration
Day 0
Day 0
Day 07
Day 07
30Day 0790
Rabies immunoglobulin
•Passive antibody is present 24 hours after injection
•Half-life of approximately 21 days.
•Dosage
–HRIG 20 IU/kg
–ERIG 40 IU/kg,
admin as soon as possible at the same time as vaccine, or up to 7
days after vaccine inj.
HRIG 300 IU/2ml ~ 4000 baht
(1 vial / 15 kg BW)
ERIG 1000IU/5ml~ 1900 baht
(1 vial / 25 kg BW)
•Passive antibody is present 24 hours after injection
•Half-life of approximately 21 days.
•Dosage
–HRIG 20 IU/kg
–ERIG 40 IU/kg,
admin as soon as possible at the same time as vaccine, or up to 7
days after vaccine inj.
HRIG 300 IU/2ml ~ 4000 baht
(1 vial / 15 kg BW)
ERIG 1000IU/5ml~ 1900 baht
(1 vial / 25 kg BW)
Should not inject RIG
•Later than 7 days after the initiation of
post-exposure vaccination.
•Previously immunized
as this may reduce the immunologic response
to the vaccine.
•Later than 7 days after the initiation of
post-exposure vaccination.
•Previously immunized
as this may reduce the immunologic response
to the vaccine.
Precuation
•RIG may interfere with the body's immune
response to certain live virus vaccines such as
measles, mumps, and rubella, should be
administered at least 14 days prior to, or at least
3 months after administration of RIG
•If IM inj is contra-indicated, inj may be given by
SC with pressure and compress applied to site
after inj.
•Do not exceed recommended doses as this may
reduce the immune response to rabies vaccine.
•RIG may interfere with the body's immune
response to certain live virus vaccines such as
measles, mumps, and rubella, should be
administered at least 14 days prior to, or at least
3 months after administration of RIG
•If IM inj is contra-indicated, inj may be given by
SC with pressure and compress applied to site
after inj.
•Do not exceed recommended doses as this may
reduce the immune response to rabies vaccine.
Previously immunized person
•2 IM / ID doses
–Day 0 and day 3
• RIG should not be given.
Full PEP should be given to persons :
–who received pre-or post-exposure prophylaxis with
vaccines of unproven potency
–patients whom immunological memory is not longer
assured as a result of HIV/AIDS or other immunosupp
ressive causes
•2 IM / ID doses
–Day 0 and day 3
• RIG should not be given.
Full PEP should be given to persons :
–who received pre-or post-exposure prophylaxis with
vaccines of unproven potency
–patients whom immunological memory is not longer
assured as a result of HIV/AIDS or other immunosupp
ressive causes
OPD or IPD
I am a
Pit bull
Pit bull
Another pit bull attack
Rabies
• A viral, zoonotic
neroinvasive disease
•Mortality rate of 100%
35,000-50,000 deaths
annually worldwide
• A viral, zoonotic
neroinvasive disease
•Mortality rate of 100%
35,000-50,000 deaths
annually worldwide
Transmission
•Humans most often become infected with rabies through
the bite or scratch of an infected dog or cat.
•Routes of transmission have been documented and
include contamination of mucous membranes (i.e., eyes,
nose, mouth), aerosol transmission, and corneal
transplantations
•Rabies virus can be excreted in the saliva of infected
animals several days before illness is apparent
•Humans most often become infected with rabies through
the bite or scratch of an infected dog or cat.
•Routes of transmission have been documented and
include contamination of mucous membranes (i.e., eyes,
nose, mouth), aerosol transmission, and corneal
transplantations
•Rabies virus can be excreted in the saliva of infected
animals several days before illness is apparent
•Figure 2. The cycle of rabies infection begins with viral entry at a peripheral site and
proceeds through retrograde axonal transport. Viral replication occurs in the cell body
of the primary neuron. Infection proceeds by transsynaptic spread through several
neurons before spreading to the acinar cells, which then shed the virus into the saliva
(Dietzschold et al. 2005).
proceeds through retrograde axonal transport. Viral replication occurs in the cell body
of the primary neuron. Infection proceeds by transsynaptic spread through several
neurons before spreading to the acinar cells, which then shed the virus into the saliva
(Dietzschold et al. 2005).
Rabies virus
•Rabies virus travels along axons at a rate of
12-24 mm/d* to enter the spinal ganglion
•From here, the rabies virus spreads quickly, at a
rate of 200-400 mm/d* into the CNS
•Average incubation is 20-90 days.
–> 90% of cases, incubation is less than 1 year
–Rarely, incubation lasts as long as 19 years.
*http://emedicine.medscape.com
•Rabies virus travels along axons at a rate of
12-24 mm/d* to enter the spinal ganglion
•From here, the rabies virus spreads quickly, at a
rate of 200-400 mm/d* into the CNS
•Average incubation is 20-90 days.
–> 90% of cases, incubation is less than 1 year
–Rarely, incubation lasts as long as 19 years.
*http://emedicine.medscape.com
Test for rabies
•Rabies diagnosis in animals(after the animal is dead).
–Direct Fluorescent Antibody (DFA) is the “gold standard” diagnostic method for
rabies
–Tissue from at least two locations in the brain, preferably the brain stem and
cerebellum.
•Rabies diagnosis in humans
–Tests are performed on samples of saliva, serum, spinal fluid.
–Skin biopsy specimens are examined for rabies antigen in the
cutaneous nerves at the base of hair follicles
•Rabies virus is not found in blood, urine, or feces.
•Rabies diagnosis in animals(after the animal is dead).
–Direct Fluorescent Antibody (DFA) is the “gold standard” diagnostic method for
rabies
–Tissue from at least two locations in the brain, preferably the brain stem and
cerebellum.
•Rabies diagnosis in humans
–Tests are performed on samples of saliva, serum, spinal fluid.
–Skin biopsy specimens are examined for rabies antigen in the
cutaneous nerves at the base of hair follicles
•Rabies virus is not found in blood, urine, or feces.
Symptoms
Incubation period ( 20-90 day)
asymptomatic
Prodromal period (enters the CNS, 2-10 day)
fever malaise anorexia headaches
nausea emesis
oagitation diarrhea
Neurologic period (objective signs of
developing CNS disease , 2-7 days)
psychosis, restlessness ,seizures, aphasia
hydrophobia and aerophobia
signs of cranial nerve involvement: diplopia
facial palsy, and optic neuritis
Coma and death
Incubation period ( 20-90 day)
asymptomatic
Prodromal period (enters the CNS, 2-10 day)
fever malaise anorexia headaches
nausea emesis
oagitation diarrhea
Neurologic period (objective signs of
developing CNS disease , 2-7 days)
psychosis, restlessness ,seizures, aphasia
hydrophobia and aerophobia
signs of cranial nerve involvement: diplopia
facial palsy, and optic neuritis
Coma and death
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