Read Rosen & Barkin's 5-Minute Emergency Medicine Consult Online

Authors: Jeffrey J. Schaider,Adam Z. Barkin,Roger M. Barkin,Philip Shayne,Richard E. Wolfe,Stephen R. Hayden,Peter Rosen

Tags: #Medical, #Emergency Medicine

Rosen & Barkin's 5-Minute Emergency Medicine Consult (595 page)

BOOK: Rosen & Barkin's 5-Minute Emergency Medicine Consult
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PRE HOSPITAL
  • Thoroughly wash wound with soap and water.
  • If safely able, capture wild animal for sacrifice and testing.
INITIAL STABILIZATION/THERAPY
  • Airway, breathing, and circulation
  • Intubation as needed
  • Treatment of seizures
ED TREATMENT/PROCEDURES
  • Wound cleansing and irrigation
  • Tetanus immunization
  • Determine if exposure requires prophylaxis:
    • Consult local health department
    • Domestic animal bite:
      • Home monitoring of animal for 10 days
      • If animal displays no signs of illness, patient does not need PEP.
    • Wild animal bite:
      • Rabies testing of sacrificed animal head-Negri bodies are diagnostic
      • Start PEP and stop if test is negative
      • Treat if animal not captured.
    • Unprovoked attacks should be assumed high risk for exposure.
  • PEP:
    • Passive immunization with human rabies immune globulin (HRIG)
    • HRIG: 20 IU/kg:
      • Majority infiltrated in and around wound
      • Remainder given IM (gluteus)
      • Active immunization with rabies vaccine
    • Rabies vaccine: 1 mL (2.5 IU) IM days 0, 3, 7, 14, add day 28 if immunocompromised
    • 3 vaccines approved in US:
      • Imovax–human diploid cell culture
      • RabAvert–chick embryo cell culture
      • Rabies vaccine adsorbed–inactivated virus, for US military
    • Administration location:
      • Deltoid in adults or anterior thigh in small children or infants
  • For those with pre-exposure prophylaxis and rabies exposure:
    • Do not require HRIG
    • Need vaccine booster on days 0 and 3
  • If care delayed after rabies exposure:
    • HRIG not indicated >7 days after exposure
    • Vaccine should be administered as usual
  • Pre-exposure prophylaxis:
    • Rabies vaccine on days 0, 7, 21, 28
    • Target groups: Veterinarians, animal handlers, virus lab workers, foreign travelers in endemic regions
Pediatric Considerations

Treat as in adults.

Pregnancy Considerations

Treatment considered safe during pregnancy.

FOLLOW-UP
DISPOSITION

Ensure adequate access for subsequent vaccine administration post rabies exposure.

Admission Criteria

Patient with clinical signs of rabies

Discharge Criteria
  • Stable patient
  • No evidence of reaction to vaccine
Issues for Referral

Public health and CDC for suspicious cases

FOLLOW-UP RECOMMENDATIONS
  • Ensure access to subsequent vaccine doses
  • Patient should follow up with animal control if source animal has been sacrificed or is being observed.
PEARLS AND PITFALLS
  • PEP is only proven treatment after exposure.
  • PEP should be given in all high-risk exposures regardless of timing
  • Vaccine should only be given in deltoid in adults: Treatment failures reported with inadvertent SC administration in gluteus injections.
ADDITIONAL READING
  • American Academy of Pediatrics.
    Report of the Committee on Infectious Report
    . 29th ed. Elk Grove Village, IL: American Academy of Pediatrics; 2012.
  • Centers for Disease Control and Prevention. Rabies. Available at
    http://www.cdc.gov/rabies./
    Updated December 13, 2012.
  • Centers for Disease Control and Prevention (CDC). Recovery of a patient from clinical rabies–California, 2011.
    MMWR Morb Mortal Wkly Rep.
    2012;61(4):61–65.
  • Franka R, Rupprecht CE. Treatment of rabies in the 21st century: Curing the incurable.
    Future Microbiol.
    2011;6:1135–1140.
  • Manning SE, Rupprecht CE, Fishbein D, et al. Human rabies prevention—United States, 2008: Recommendations of the Advisory Committee on Immunization Practices.
    MMWR Recomm Rep
    . 2008;57:1–28.
  • Willoughby RE Jr, Tieves KS, Hoffman GM, et al. Survival after treatment of rabies with induction of coma.
    N Engl J Med.
    2005;352:2508–2514.
See Also (Topic, Algorithm, Electronic Media Element)
  • Encephalitis
  • Meningitis
CODES
ICD9
  • 071 Rabies
  • V01.5 Contact with or exposure to rabies
ICD10
  • A82.9 Rabies, unspecified
  • Z20.3 Contact with and (suspected) exposure to rabies
RADIATION INJURY
Robert J. Feldman
BASICS
DESCRIPTION
  • Radiation
    in this chapter refers to ionizing radiation.
  • Alpha (
    α
    )—helium nucleus; does not penetrate skin
  • Beta (
    β
    )—electron; penetrates tissue a few cm
  • Gamma (
    γ
    )—photon; penetrates body
  • Neutron—very penetrating; not detected by Geiger counter, but neutron emitters
    also emit γ radiation
  • Radioisotope/radionuclide—chemical element that emits radiation from its nucleus:
    • Radioactivity cannot be destroyed, only relocated or shielded.
    • Being radioactive does not change element’s other chemical and physical properties, such as heavy metal toxicity.
  • Exposure/irradiation—patient has been in presence of ionizing radiation:
    • Whole body or only certain areas may be exposed.
  • Contamination—radioactive material where it is not desired:
    • Internal—within body (e.g., lung)
    • External—outside body (skin, hair, clothing)
  • Dose—amount of radiation energy absorbed by tissue:
    • Units and conversions:
      • 1 gray (Gy) = 100 rad
      • 1 sievert (Sv) = 100 rem
    • For β and γ radiation:
      • 1 Gy = 1 Sv = 100 rad = 100 rem
ALERT

Contact regional or federal authorities for guidance if radiation incident is suspected.

Pediatric Considerations
  • Children are more sensitive to radiation injury.
  • Potassium iodide is most protective for children and should be given promptly if contamination with radioactive iodine (I-131) is suspected.
Pregnancy Considerations
  • Developing fetus is very sensitive to radiation.
  • Pregnant staff should not care for radioactively contaminated patients.
ETIOLOGY
  • Ionizing radiation leads to cellular injury.
  • Damage to blood vessels leads to endarteritis and loss of tissue blood supply.
  • Higher rates of cell division within an organ make it more sensitive to radiation:
    • Bone marrow and GI tract are very sensitive.
    • Skin and nerve are less sensitive.
  • Acute radiation syndrome
    (ARS) occurs in stages following whole-body exposure:
    • Prodromal: Acute radiation injury leads to acute inflammation (0–48 hr).
    • Latent: If the acute phase of injury is survived, inflammation and symptoms subside (0–2 wk).
    • Manifest illness: At higher radiation doses, organ failure then develops.
    • Recovery or death (usually from infection) follows.
  • Sources of radiation include medical devices, therapeutics, nuclear weapons, and industry.
DIAGNOSIS
  • Diagnosing contamination is fairly easy.
  • Diagnosing and quantifying exposure is more difficult and probably require expert consultation.
SIGNS AND SYMPTOMS
  • Vary based on dose; see:
    http://www.afrri.usuhs.mil/outreach/pdf/AFRRI-Pocket-Guide.pdf
    for quick reference.
  • Overall:
    • Whole-body exposure: Syndrome similar to high-dose chemotherapy toxicity
    • ARS progresses more rapidly the higher the absorbed dose.
  • Local exposure:
    • Early resembles thermal or UV burn
    • Later resembles ischemic ulcer
BOOK: Rosen & Barkin's 5-Minute Emergency Medicine Consult
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