Rosen & Barkin's 5-Minute Emergency Medicine Consult (327 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
  • 466.0 Acute bronchitis
  • 491.9 Unspecified chronic bronchitis
  • 786.30 Hemoptysis, unspecified
ICD10
  • J20.9 Acute bronchitis, unspecified
  • J42 Unspecified chronic bronchitis
  • R04.2 Hemoptysis
HEMORRHAGIC FEVERS
Fraser C. Mackay

Ben Osborne
BASICS
DESCRIPTION

Hemorrhagic fever
describes a multisystem syndrome of vasocapillary permeability and/or organ dysfunction. Viral hemorrhagic fever (VHF) is caused by a distinct group of viruses, but the initial phase resembles influenza-like illness. Hemorrhagic stages typify the minority of patients and the later phases of disease.

RISK FACTORS
  • Travel in endemic region
  • Biologic warfare
  • Close animal contact, insect bite or ingestion
PATHOPHYSIOLOGY
  • VHF causes endothelial damage and increase vascular permeability, hemorrhage, and may proceed to shock
  • VHF shock state is both hypovolemic and distributive, and is often very difficult to reverse. Hypotension can progress swiftly, and indicates very high mortality.
  • DIC appears to be a regular feature of Marburg and Crimean-Congo hemorrhagic fever but is less frequent with Arenavirus infections.
  • Dengue hemorrhagic fever is immune mediated and is usually the result of secondary infection. It is among the most common causes for VHF.
ETIOLOGY
  • RNA viruses that have zoonotic life cycles in specific geographic areas
  • Short incubation period (<10–21 days)
  • More common VHF vectors:
    • Filoviruses: Fruit bat reservoir, unclear mode of transmission (sub-Saharan Africa)
      • Ebola
      • Marburg
    • Arenaviruses: Rodent reservoir, aerosolized rodent excreta (sub-Saharan Africa).
      • Lassa
      • South American hemorrhagic fevers
    • Flaviviruses: Human reservoir, via mosquito (tropics, increasingly worldwide)
      • Dengue (common cause of VHF)
      • Yellow fever
    • Bunyaviridae: Rodent reservoir, via tick or mosquito (Europe, South Asia, Africa)
      • Rift Valley fever
      • Crimean-Congo hemorrhagic fever
    • Hantaviridae: Rodent reservoir, aerosolized rodent excreta (Southwest USA)
      • Hemorrhagic fever with renal syndrome
      • Hantavirus pulmonary syndrome
ALERT
  • Potential biowarfare threat:
    • Aerosols (with exception of dengue) and body fluids highly infectious
    • High morbidity/mortality in some cases
    • Replicate well in cell culture, permitting weaponization
DIAGNOSIS
SIGNS AND SYMPTOMS
  • Most common (>50%) symptoms:
    • Acute febrile illness
    • Malaise
    • Headache
    • Nausea/vomiting
    • Flushing
    • Diarrhea (nonbloody)
    • Abdominal pain
    • Myalgias
  • Less common (<30%) symptoms:
    • Gingival hemorrhage
    • Conjunctival injection/hemorrhage
    • Petechia
    • Hematemesis
    • Melena
    • Epistaxis
    • Ecchymoses
  • Hemorrhagic presentations >3 days into disease
    • Skin, IV sites, gums, nose, lungs, GI tract, or uterus
    • Diffuse alveolar hemorrhage or ARDS
    • More common in CCHF, Lassa, Marburg, Ebola, Hantavirus
  • Exanthems
    • Marburg and Ebola: Nonpruritic centripetal, papular, erythematous eruption appearing between days 5 and 7, which then coalesce into well-demarcated macules that may be hemorrhagic
    • Yellow fever: Jaundice
    • Dengue: Bright maculopapular truncal erythroderma that blanches dramatically under light pressure (often on lower extremities)
  • Hemodynamic collapse, shock, seizures, coma, death.
    • Late stage of disease, often irreversible
History
  • Travel to endemic regions
  • Sick contacts
  • Clustering of cases should raise concerns of a bioweapon attack or outbreak
Physical-Exam
  • Protection of health care workers:
    • Universal blood and body precautions
  • Vital signs: Monitor BP, fever, tachycardia
    • Narrowed pulse pressure (<20 mm Hg) may signal imminent cardiovascular collapse
  • Hemorrhage (see Signs and Symptoms)
  • Exanthems (see Signs and Symptoms)
  • RUQ tenderness or hepatomegaly
    • Hepatitis
  • Adventitious lung sounds
ESSENTIAL WORKUP
  • Focus on differentiating from other acute febrile illnesses, especially in the traveler.
  • Investigate lung involvement, as it can indicate systemic disease and worse outcome
  • Recognize possible biologic attack when unusual number of patients present with similar and/or unusual findings.
  • History to identify potential pathogen:
    • Include recent travel, illnesses, or other sources of exposure.
    • Often patients are unaware of animal contacts
DIAGNOSIS TESTS & NTERPRETATION
Lab
  • CBC:
    • May see leukocytosis, leukopenia, thrombocytopenia, or pancytopenia
    • Abnormally high hematocrit can signify hemoconcentration; may indicate increased 3rd spacing impending shock/cardiovascular collapse.
  • Electrolytes, BUN, creatinine, and glucose levels:
    • Consider renal failure
  • Liver function tests:
    • Hepatic involvement is common, but jaundice occurs mainly with yellow fever.
  • Type and screen, prothrombin time, partial thromboplastin time, and
    d
    -dimer tests:
    • Look for coagulopathy and DIC (seen in Crimean-Congo hemorrhagic fever, Ebola, and Marburg)
  • Special lab test:
    • In specialized labs (biohazard level 4), definitive diagnosis can be made by viral isolation, real-time reverse transcriptase polymerase chain reaction (RT-PCR), and immunohistochemistry techniques:
      • Coordinated with CDC
      • Thick and thin smears to help differentiate from malaria
Imaging

CXR, head, and abdominal CT scanning:

  • Rule out pneumonia or ARDS
  • Intracranial and intra-abdominal bleeding
Diagnostic Procedures/Surgery

Serum and saliva can be analyzed by RT-PCR in specialized labs.

DIFFERENTIAL DIAGNOSIS
  • Malaria:
    • A concern for traveler with fever
  • Dengue fever:
    • Common source of fever in traveler
  • Rickettsial:
    • Rocky Mountain spotted fever
    • Typhus
  • Bacterial:
    • Meningococcemia
    • Sepsis
    • EHEC (Escherichia coli O157:H7)
  • Systemic disease:
    • Leukemia
    • TTP, ITTP
  • Pit viper envenomation
TREATMENT
PRE HOSPITAL
ALERT
  • Increasing globalization has increased frequency of imported cases of rare diseases.
  • Early detection of VHF, natural, or biologic attack is key to control an outbreak. Report to CDC.
  • Most cases will derive from patients who traveled to or had contact with persons from parts of the world where the viruses are endemic.
INITIAL STABILIZATION/THERAPY

Protection of health care workers:

  • Universal blood and body precautions
  • Isolation of patient
  • Use of protective clothing plus HEPA-filtered respirators to minimize exposure to aerosols for those involved in procedures such as suctioning, catheter placement, and wound dressing
ED TREATMENT/PROCEDURES
  • Supportive therapy
  • Empiric therapy with antimalarial regimens until definitive diagnosis is obtained
  • Aggressive treatment of secondary infections
  • Bleeding is usually mild, and life-threatening blood loss is rare:
    • If indicated, hemorrhage can be managed by replacement of blood, platelets, and clotting factors.
  • Fluid support
    • Patients are prone to 3rd spacing and can go into flash pulmonary edema; be judicious with crystalloids.
    • Reserve colloids/blood products for impending shock/cardiovascular collapse.
  • Ribavirin—a synthetic nucleoside:
    • Useful for Lassa, South American hemorrhagic fever, Crimean-Congo hemorrhagic fever, and hemorrhagic fever with renal syndrome; ineffective against filoviruses
    • Causes a reversible hemolytic anemia
  • Transfusion of immune plasma (convalescent plasma therapy) for South American hemorrhagic fever within 1st week of symptoms

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