Rosen & Barkin's 5-Minute Emergency Medicine Consult (216 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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Potential – MS, MG, stroke, aneurysm, SAH, lymphocytic meningitis, Wernicke encephalopathy

CODES
ICD9
  • 368.2 Diplopia
  • 368.15 Other visual distortions and entoptic phenomena
ICD10

H53.2 Diplopia

DISSEMINATED INTRAVASCULAR COAGULATION
Steven H. Bowman

Ernesto J. Romo
BASICS
DESCRIPTION
  • Normal coagulation: Series of local reactions among blood vessels, platelets, and clotting factors
  • Disseminated intravascular coagulation (DIC) is systemic activation of coagulation and fibrinolysis by some other primary disease process.
  • Coagulation system activation results in systemic circulation of thrombin and plasmin.
  • Role of thrombin in DIC:
    • Tissue factor/factor VIII(a) activate the extrinsic pathway, leads to thrombin formation.
    • Thrombin circulates and converts fibrinogen to fibrin monomer.
    • Fibrin monomer polymerizes into fibrin (clot) in the circulation.
    • Clots cause microvascular and macrovascular thrombosis with resultant peripheral ischemia and end organ damage.
    • Platelets become trapped in clot with resultant thrombocytopenia.
  • Role of plasmin in DIC:
    • Plasmin circulates systemically converting fibrinogen into fibrin degradation products (FDPs).
    • FDPs combine with fibrin monomers.
    • FDP-monomer complexes interfere with normal polymerization and impair hemostasis.
    • FDPs also interfere with platelet function.
  • Role of impaired anticoagulation in DIC.
    • Failure of physiologic anticoagulation is necessary for DIC to occur.
    • Antithrombin III, protein C system, and tissue factor pathway inhibitor all impaired.
  • Acute DIC—uncompensated form:
    • Clotting factors used more rapidly than body can replace them
    • Hemorrhage
      predominant clinical feature, which overshadows ongoing thrombosis
  • Chronic DIC—compensated form:
    • Body able to keep up with pace of clotting factor consumption
    • Thrombosis
      predominant clinical feature
ETIOLOGY
  • Precipitated by many disease states
  • Complications of pregnancy:
    • Retained fetus
    • Amniotic fluid embolism
    • Placental abruption
    • Abortion
    • Eclampsia
    • HELLP syndrome
  • Sepsis:
    • Gram negative (endotoxin-mediated meningococcemia)
    • Gram positive (mucopolysaccharide-mediated)
    • Other microorganisms (e.g., viruses, parasites)
  • Trauma:
    • Crush injury
    • Severe burns
    • Severe head injury
    • Fat embolism
  • Malignancy:
    • Solid tumor or metastatic disease
    • Hematologic malignancy (e.g., leukemia)
  • Intravascular hemolysis:
    • Transfusion reactions
    • Massive transfusion
  • Organ destruction:
    • Severe pancreatitis
    • Severe hepatic failure
  • Vascular abnormalities:
    • Kasabach–Merritt syndrome
    • Large vascular aneurysm
  • Thrombocytopenia:
    • Thrombotic thrombocytopenic purpura
    • Idiopathic thrombocytopenic purpura
  • Miscellaneous:
    • Snake bites
    • Recreational drugs
DIAGNOSIS
SIGNS AND SYMPTOMS
  • Excessive bleeding:
    • Petechiae
    • Purpura
    • Hemorrhagic bullae
    • Wound bleeding
    • Bleeding from venipuncture/arterial lines
    • Epistaxis
    • Hemoptysis
    • GI bleeding
  • Excessive thrombosis:
    • Large vessels
    • Microvascular thrombosis and end organ dysfunction
    • Cardiac, pulmonary, renal, hepatic, CNS
    • Thrombophlebitis
    • Pulmonary embolus
    • Nonbacterial thrombotic endocarditis
    • Gangrene
    • Ischemic infarcts of kidney, liver, CNS, bowel
  • Acute DIC:
    • Hemorrhagic complications predominate.
  • Chronic DICL:
    • Thrombotic complications predominate.
History
  • Previous history of bleeding disorder
  • Pregnancy/last menstrual period
  • History of malignancy or immunocompromised
Physical-Exam
  • Neurologic:
    • Altered MS, confusion, lethargy
  • Cardiovascular:
    • Hypotension, tachycardia
  • Respiratory:
    • Tachypnea, rhonchi, rales
  • GI:
    • Upper or lower GI bleeding, abdominal distension
  • GU:
    • Oliguria, hematuria
  • Skin:
    • Petechiae, purpura, jaundice, necrosis
ESSENTIAL WORKUP
  • Depends on precipitating illness
  • Diagnosis generally not made in ED
DIAGNOSIS TESTS & NTERPRETATION
Lab
  • Platelet count:
    • Important to note rapid decrease
    • <100,000/mm
      3
    • May be normal in chronic DIC
  • Prothrombin time (PT)/partial thromboplastin time (PTT):
    • Increased
    • May be normal in chronic DIC
  • Fibrinogen:
    • Decreased
    • <150 mg/dL in 70%
    • Low sensitivity, as levels can remain normal
    • May be normal in chronic DIC
  • FDPs:
    • Increased
    • >40 μg/mL
  • D-dimer increased
  • CBC/peripheral smear:
    • Red cell fragments
    • Low platelets
    • Peripheral smear confirms disease in chronic DIC
  • Electrolytes, BUN, creatinine, glucose:
    • Elevated BUN, creatinine owing to renal insufficiency
  • ABGs:
    • Oxygen, acid–base status
  • ISTH scoring system
    • Underlying disorder associated with DIC
      • no = 0, yes = 2
    • Platelet count
      • >100 = 0, <100 = 1, <50 = 2
    • Fibrin markers (D-dimer, FDP)
      • Normal = 0, moderate increase = 1, strong increase = 2
    • Prolonged PT
      • <3 = 0, >3 but <6 = 1, >6 = 2
    • Fibrinogen
      • 1 g/L = 0, <1 g/L = 1
    • Score >5 overt DIC, associated with increased mortality.
Imaging
  • CXR for suspected pneumonia
  • Head CT for altered mental status
  • OB US in pregnant patients
DIFFERENTIAL DIAGNOSIS
  • Inherited coagulation disorders:
    • Factor deficiencies
  • Other acquired coagulation disorders:
    • Anticoagulant therapy
    • Drugs
    • Hepatic disease
    • Vitamin K deficiency
    • Massive blood loss
  • Platelet dysfunction:
    • TTP/HUS
    • HIT
    • ITP
  • Platelet dysfunction:
    • TTP/HUS
    • HI
TREATMENT
INITIAL STABILIZATION/THERAPY
  • Airway management and resuscitation measures:
    • Control bleeding
    • Establish IV access
    • Restore and maintain circulating blood volume.
  • Initiate therapy of precipitating disease:
    • Antibiotics in sepsis
    • Evacuate uterus of retained products of conception
    • Chemotherapy in malignancy
    • Débridement of devitalized tissue in trauma
ED TREATMENT/PROCEDURES
  • Therapy of DIC is controversial and should be individualized based on:
    • Age
    • Hemodynamic status
    • Severity of hemorrhage
    • Severity of thrombosis
  • Involve admitting service before initiating specific DIC therapy.
  • Replace depleted blood components:
    • Fresh frozen plasma (FFP):
      • For prolonged PT
      • Provides clotting factors and volume replacement
      • Dose: 2 U or 10–15 mL/kg
    • Platelets:
      • If platelet count <20,000 or platelet count <50,000 with ongoing bleeding
      • Dose: 1 U/10 kg body weight
    • Cryoprecipitate:
      • Higher fibrinogen content than whole plasma
      • For severe hypofibrinogenemia (<50 mg/dL) or for active bleeding with fibrinogen <100 g/dL
      • Dose: 8 U
    • Recombinant factor VIIa
      • Successful use reported, benefit and safety unknown.
    • Washed packed cells
    • Albumin
    • Nonclotting volume expanders
  • Inhibit intravascular clotting with heparin:
    • Use is controversial.
    • Consider when thrombosis predominates.
    • May be effective in mild to moderate DIC
    • Efficacy undetermined in severe DIC. Possible indications:
      • Purpura fulminans (gangrene of digits, extremities)
      • Acute promyelocytic leukemia
      • Dead fetus syndrome—several weeks after intrauterine fetal death
      • Thromboembolic complications of large vessels
      • Before surgery with metastatic carcinoma
    • Administer activated protein C (controversial):
      • No mortality benefit.
    • Antithrombin
      • No mortality benefit found in patients also receiving heparin.
      • Lack of evidence to support use at this time.
  • Inhibit fibrinolysis:
    • Block secondary compensatory fibrinolysis that accompanies DIC
    • Use complicated by severe thrombosis
    • Use only when DIC accompanied by primary fibrinolysis:
      • Promyelocytic leukemia
      • Giant hemangioma
      • Heat stroke
      • Amniotic fluid embolism
      • Metastatic carcinoma of prostate
    • Initiate in extreme cases only:
      • Profuse bleeding not responding to replacement therapy
      • Excessive fibrinolysis present (rapid whole blood lysis/short euglobulin lysis time)
      • E
        -
        aminocaproic acid (EACA)
      • Tranexamic acid

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