Rosen & Barkin's 5-Minute Emergency Medicine Consult (252 page)

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

Tags: #Medical, #Emergency Medicine

BOOK: Rosen & Barkin's 5-Minute Emergency Medicine Consult
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CODES
ICD9

784.7 Epistaxis

ICD10

R04.0 Epistaxis

ERYSIPELAS
Irving Jacoby
BASICS
DESCRIPTION
  • Superficial bacterial infection of the skin with prominent lymphatic involvement
  • Leukocytosis is common
  • Positive blood cultures in 3–5%
ETIOLOGY
  • Group A β-hemolytic streptococcus is the causative organism (uncommonly, group C or G streptococci)
  • Portals of entry:
    • Skin ulcers
    • Local trauma
    • Abrasions
    • Psoriatic or eczematous lesions
    • Fungal infections
Pediatric Considerations
  • Haemophilus influenzae
    type b (HIB) causes facial cellulitis in children that may appear similar to erysipelas:
    • Should be considered in unimmunized children
    • Many will be bacteremic and require admission
    • Cefuroxime or other appropriate
      H. influenzae
      coverage is important
    • H. influenzae
      is much less common since widespread use of the HIB vaccine
  • Group B streptococci can cause erysipelas in the newborn
  • Can develop from infection of umbilical stump
Pregnancy Considerations
  • Erythema of the breast in puerperal mastitis is often caused by Staphylococcus organisms, hence methicillin-resistant
    S. aureus
    (MRSA) should be covered
    • See Mastitis
DIAGNOSIS
SIGNS AND SYMPTOMS
  • Most common sites of involvement are the face (5–20% of cases), lower legs (70–80% of cases), and ears
  • Skin has an intense fiery red color, hence the name “Saint Anthony’s fire”
  • Often bilateral on the face, but unilateral elsewhere
  • Predilection for infants, children, and the elderly
  • Systemic symptoms may include malaise, fever, chills, nausea, and vomiting
  • Traumatic portal of entry on skin is not always apparent
  • Rarely there may be an associated periorbital cellulitis or cavernous sinus involvement
History
  • Facial erysipelas may follow a nasopharyngeal infection or trauma
  • Predilection for areas of lymphatic obstruction:
    • Particularly in the upper extremity following radical mastectomy
    • Increased frequency after saphenous vein harvesting or stripping
    • May be a marker for previously undiagnosed lymphatic obstruction, or patients with congenital lymphedema (such as Milroy disease)
  • 30% recurrence rate within 3 yr, owing to lymphatic obstruction caused by an episode of erysipelas
Physical-Exam
  • Involved skin is:
    • Edematous
    • Indurated (peau d’orange)
    • Painful
    • Well-circumscribed plaque with sharp, clearly demarcated edges
  • Classical butterfly rash on cheeks and across nose when affecting face
  • Vesicles and bullae may be present in more serious infections
ESSENTIAL WORKUP
  • The diagnosis is clinical:
    • Based on the characteristic skin findings and the clinical setting
  • Needle-aspirate wound cultures are seldom positive and not indicated
DIAGNOSIS TESTS & NTERPRETATION
Lab
  • Swabs of the skin are not indicated for culture, as they will show only skin organisms
  • CBC with differential, and blood cultures should be performed in diabetics and other high-risk populations, or in patients with hypotension and those who require admission:
    • Blood cultures more likely to be positive in patients with lymphedema
  • Check glucose in diabetics as infection may disrupt control
  • Urinalysis: To check for proteinuria, hematuria, and red cell casts
    • Would suggest diagnosis of post-streptococcal glomerulonephritis (PSGN)
    • If it occurs, usually around 2 wk after onset of skin infection
  • Antistreptolysin O (ASL-O), anti-DNase B and streptolysin antibody serial titer changes are useful in diagnosing post-streptococcal immunologic entities such as rheumatic fever or glomerulonephritis,
    • Do not add anything to the diagnosis and management of uncomplicated erysipelas
    • Should not be routinely ordered unless there are already manifestations of such complications
Imaging
  • There is no standard imaging for classical erysipelas
    • If deeper infection such as myositis is suspected, plain films of an extremity or CT scan may be performed to assess for the presence of gas
  • Ultrasound may be useful to evaluate for an abscess if this is suspected, or in the leg to r/o deep vein thrombophlebitis DVT
DIFFERENTIAL DIAGNOSIS
  • Abscess
  • Acute bacterial sinusitis
  • Allergic inflammation
  • Cellulitis
  • Contact dermatitis
  • DVT
  • Diffuse inflammatory carcinoma of the breast
  • Familial mediterranean fever
  • Herpes zoster, second division of cranial nerve V
  • Impetigo
  • Inflammatory dermatophytosis
  • Mastitis
  • Necrotizing fasciitis
  • Periorbital cellulitis
  • Systemic lupus erythematosus (SLE) with butterfly rash
  • Streptococcal or staphylococcal TSS (sunburn-like rash)
  • Venous stasis dermatitis
  • Viral exanthem
TREATMENT
PRE HOSPITAL

Wearing gloves, followed by hand washing when managing patients, to decrease risk of transmission of streptococcal carriage

INITIAL STABILIZATION/THERAPY

Patients may be toxic and in need of intravenous fluid resuscitation or pressure support

ED TREATMENT/PROCEDURES
  • Appropriate antibiotic therapy; treatment should be for 10 days:
    • Patients with extensive involvement should be admitted for parenteral antibiotic treatment
    • May switch to oral antibiotics when patient is stable and showing signs of response
  • Mild cases: Patients can be discharged on oral therapy if nontoxic appearing, good compliance, and close follow-up can be ensured
  • Penicillin is the drug of choice when symptoms are consistent with erysipelas
  • If there is difficulty in distinguishing from cellulitis, staphylococcal coverage should be added:
    • Use penicillinase-resistant penicillin or 1st-generation cephalosporin
    • If in community with high incidence of MRSA, use vancomycin, or other anti-MRSA coverage
    • Reports of vancomycin-resistant Staphylococci are occurring
  • Acetaminophen for fever
  • Isolation while in hospital
    • Contagious
MEDICATION

OUTPATIENT

  • Penicillin V: 500 mg PO q6h (peds: 25–50 mg/kg/d div. q6–8h) for 10 days.
  • Amoxicillin: 500 mg PO q8h (peds: 50 mg/kg/d div. TID) for 10 days.
  • Clindamycin: 300 mg PO QID (peds: 8–25 mg/kg/d suspension PO div. TID or QID) for 10 days.
  • Dicloxacillin: 500 mg PO q6h (peds: 30–50 mg/kg/d PO div. q6h) for 10 days
  • Erythromycin: 250–500 mg PO q6h (peds: 40 mg/kg/d PO in div. doses q6h) for 10 days
  • Cephalexin: 500 mg PO q6h (peds: 40 mg/kg/d PO div. q8h) for 10 days
  • Cefuroxime: 250–500 mg PO BID (peds: 30 mg/kg/d PO div. q12h) for 10 days.

INPATIENT

  • Penicillin G: 2 million U q4h IV (peds: 25,000 U/kg IV q6h).
  • Penicillin G, procaine: 600,000 U q12h IM
  • Clindamycin: 600 mg q8h IV (peds: 20–40 mg/kg/d IV div. q8h)
  • Vancomycin: 1 g IV q12h given over 1.5–2 hr to decease risk of red man syndrome (peds: 10–15 mg/kg IV q6h)
First Line
  • Oral or IV: Penicillin or 1st-generation cephalosporin
  • Clindamycin for penicillin-allergic individuals
Second Line

Oral: Erythromycin

FOLLOW-UP
DISPOSITION

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