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Disorders of Hemostasis


Key Concepts

  • Although hemostatic disorders are confirmed through laboratory testing, a careful history and thorough physical examination may provide clues to the diagnosis.

  • The use of antithrombotic agents remains widespread, whereas diseases such as hemophilia or disseminated intravascular coagulation (DIC) are encountered infrequently in the emergency department (ED) setting.

  • Critical thrombocytopenia increases the risk of bleeding, particularly with trauma or invasive procedures. Platelet dysfunction may occur with platelet levels outside of or within the normal range. Aspirin therapy or renal disease, for instance, can cause platelet dysfunction in the setting of a normal platelet count.

  • Patients with suspected new diagnosis of immune thrombocytopenic purpura (ITP) should typically be admitted for further management; glucocorticoid therapy is the mainstay of treatment.

  • In patients with possible heparin-induced thrombocytopenia (HIT), clinical scoring systems are helpful in risk stratifying the possibility of HIT, prompting early cessation of heparin, alternative anticoagulation, and hematology consultation. Spontaneous HIT should be considered in patients following major surgery (typically an orthopedic procedure), or with recent serious infection.

  • Thrombotic thrombocytopenic purpura (TTP) should be suspected if both thrombocytopenia and microangiopathic hemolytic anemia (MAHA) are identified. Early treatment includes plasma exchange therapy.

  • Platelet transfusion is rarely indicated unless platelet counts are below 10,000/mm 3 or severe life-threatening bleeding occurs. Platelet transfusion should be avoided in the setting of thrombotic microangiopathies, such as TTP, hemolytic uremic syndrome (HUS), the “hemolysis, elevated liver function tests, and low platelets” (HELLP) syndrome complicating pregnancy, or HIT.

  • Hemophiliacs are often highly informed about their disease. It is imperative that prompt intervention with replacement therapy occurs early when bleeding or the potential for bleeding is suspected. As a general rule, 1 U/kg of factor VIII will increase the circulating factor VIII level by 2%.

  • Hemophilia with inhibitors creates a challenge for emergency resuscitation, and a treatment option is recombinant Factor VIIa.

Foundations

Hemostasis is a dynamic process that is geared to preventing blood from escaping the boundaries of the vessel. This complex process occurs in phases: maintenance of vessel integrity, formation of a platelet plug, propagation of the coagulation cascade, subsequent clot development, followed by fibrinolysis and clot disintegration. Often the steps of platelet plug formation (primary hemostasis) and the coagulation process (secondary hemostasis) are utilized interchangeably, though the processes are distinctly unique yet collaborative. Common hemostatic abnormalities are acquired and result from iatrogenic causes such as medications (e.g., aspirin, warfarin, or direct thrombin inhibitor), from disease (e.g., hepatic insufficiency), and less frequently from congenital abnormalities. Disorders of hemostasis may result in hemorrhage. Identification and expeditious treatment of the underlying cause remains paramount.

Anatomy and Physiology

Vascular integrity is maintained by a lining of overlapping endothelial cells supported by a basement membrane, connective tissue, and smooth muscle. These cells are important in maintaining a barrier to macromolecules, secreting clot-preventing substances and, when injured, in contributing to the metabolic response and local vasoconstriction. The endothelium regulates clot formation by secreting substances such as tissue factor pathway inhibitor (TFPI) and heparin sulfate, preventing propagation of the coagulation pathway, as well as prostacyclin and nitric oxide, which prevent platelet aggregation and act as vasodilators. The endothelium also expresses CD39 (cluster of differentiation 39), which degrades adenosine triphosphate (ATP) and adenosine diphosphate (ADP) to adenosine monophosphate (AMP), a potent antiplatelet and antithrombotic, and adenosine, a potent locally acting platelet inhibitor that prevents platelet plug formation ( Fig. 111.1A ). When the endothelium’s physical barrier has been compromised, exposed von Willebrand factor (vWF) links to platelet glycoprotein Ib (gpIb) receptors allowing platelet adhesion to the intravascular surface. Normal inhibitory mechanisms are disrupted through damage to the endothelial cells, allowing ATP and ADP to interact with receptors to amplify platelet activation ( Fig. 111.1B ).

Fig. 111.1, (A) The endothelium regulates clot formation through expression of a number of substances including: CD39 (cluster of differentiation 39), which degrades adenosine triphosphate (ATP) and adenosine diphosphate (ADP) to adenosine monophosphate (AMP), a potent antiplatelet and antithrombotic, and adenosine, a potent locally acting platelet inhibitor that prevents platelet plug formation. (B) When the endothelium is injured the exposed von Willebrand factor (vWF) links to platelet glycoprotein Ib (gpIb) receptors allowing platelet adhesion to the intravascular surface and allowing ATP and ADP to interact with receptors to amplify platelet activation.

Platelets have multiple roles in hemostasis. They are complex cytoplasmic fragments released from bone marrow megakaryocytes largely regulated by thrombopoietin. After initial exposure to damaged endothelium, platelets display glycoproteins to aid in adhesion and aggregation, such as gpIb and gpIIa/IIIb. Platelets also contain lysosomes, microtubules, and granules, among other components. Granules contain over 300 metabolically active substances, including platelet factor 4, additional adhesive and aggregation glycoproteins, coagulation factors, and fibrinolytic inhibitors. Each participates in the process of coagulation and contributes to overall wound healing through the mediation of inflammation, immune response, and infection control. Platelet activity is summarized in Box 111.1 . Any step in the platelet pathway may be absent, altered, or inhibited by inherited or acquired disorders. The coagulation cascade forms fibrin, and cross-linked fibrin serves to reinforce the initial platelet plug.

BOX 111.1
Role of Platelets in Hemostasis

  • 1.

    Adhesion to subendothelial connective tissue: Collagen, basement membrane, and noncollagenous microfibrils; serum factor VIII and von Willebrand factor (vWF) permit this function; adhesion creates the initial bleeding arrest plug

  • 2.

    Release of adenosine diphosphate, the primary mediator and amplifier of aggregation; release of thromboxane A, another aggregator and potent vasoconstrictor; release of calcium, serotonin, epinephrine, and trace thrombin

  • 3.

    Platelet aggregation over the area of endothelial injury

  • 4.

    Stabilization of the hemostatic plug by interaction with the coagulation system:

    • Platelet factor 3, a phospholipid that helps accelerate certain steps in the coagulation system

    • Platelet factor 4, a protein that neutralizes heparin

    • Pathway initiation and acceleration by thrombin production

    • Secretion of active forms of coagulation proteins

  • 5.

    Stimulation of limiting reactions of platelet activity

The coagulation pathway is a complex system of checks and balances that results in controlled formation of a fibrin clot. Coagulation factors are summarized in Box 111.2 , and a simplified coagulation pathway is presented in Figure 111.2 . The clotting cascade is traditionally depicted as consisting of intrinsic and extrinsic pathways. A more modern approach is to view the extrinsic pathway as the initiation phase with exposed tissue factor at the site of vessel injury, and the intrinsic pathway as a parallel and amplification pathway. Both pathways converge to activate factor X, which then converts prothrombin to thrombin. Tissue factor is a critical cofactor that is required for activation of factor VII. Because of limited amounts of tissue factor and rapid inactivation by TFPI, the extrinsic pathway initiates the clot process, though sustained generation of thrombin and clot formation is dependent on the intrinsic pathway through activation of factor IX by activated factor VII. Once coagulation is initiated, controls are necessary to prevent overzealous local or generalized thrombosis ( Box 111.3 ).

BOX 111.2
Coagulation Factors

  • Factor I. Fibrinogen

  • Factor II. Prothrombin

  • Factor III. Tissue thromboplastin

  • Factor IV. Calcium

  • Factor V. Labile factor (proaccelerin)

  • Factor VI. Not assigned

  • Factor VII. Proconvertin

  • Factor VIII. Antihemophilic A factor

  • Factor IX. Antihemophilic B factor (plasma thromboplastin component, Christmas factor)

  • Factor X. Stuart-Prower factor

  • Factor XI. Plasma thromboplastin antecedent

  • Factor XII. Hageman factor (contact factor)

  • Factor XIII. Fibrin-stabilizing factor

Fig. 111.2, Coagulation pathway.

BOX 111.3
Normal Controls of Coagulation

  • Removal and dilution of activated clotting factors through blood flow, which also mechanically opposes growth of the hemostatic plug

  • Alteration of platelet activity by endothelium-generated nitric oxide and prostacyclin

  • Removal of activated coagulation components by the reticuloendothelial system

  • Regulation of the clotting cascade by antithrombin III, protein C, protein S, and tissue factor pathway inhibitor (TFPI)

  • Activation of the fibrinolytic system

Pathophysiology

Hemostasis is dependent on normal functioning and integration of the vasculature, platelets, and coagulation pathway. The most commonly encountered disorder of hemostasis is antithrombotic drug administration, including use of antiplatelet or anticoagulant medications. Disorders of hemostasis may also be congenital, or secondary to disease states that affect the various steps of the hemostatic pathway such as malignancy or hepatic dysfunction. Due to the interconnectedness between the endothelium and platelets, vascular disorders may share similar historical or examination features with platelet disorders. Despite some overlap, disorders of hemostasis are frequently grouped into vascular disorders (often with a component of platelet dysfunction), platelet disorders, and coagulation disorders.

Clinical Features

Disorders of hemostasis may become evident through hemorrhage that is out of proportion to what would otherwise be anticipated, excessive ecchymosis, or the presence of a petechial or purpuric rash. Hemostatic disorders may complicate any medical or traumatic problem, and platelet disorders or coagulopathy can rapidly develop in critically ill patients. Patients that fail to respond to usual hemostatic measures should be considered to have a potential bleeding disorder. When a bleeding disorder is diagnosed or suggested, the assessment initially includes stabilization, which may necessitate intravenous fluids, transfusion of red blood cells (RBC), or other blood component or factor replacement. In the setting of a known disorder, clinical complications associated with the underlying pathophysiologic condition must be considered. If the disorder is unknown, a rapid differential diagnosis should be pursued.

Key components of the history and physical examination are presented in Box 111.4 . The history alone may in some cases be useful in differentiating between platelet and coagulation factor disorders.

BOX 111.4
Clinical Evaluation of a Bleeding Patient

History

  • Nature of bleeding

    • Petechiae

    • Purpura

    • Ecchymosis

    • Significant bleeding episodes

  • Sites of bleeding

    • Skin

    • Mucosa: Oral or nasal

    • Muscle

    • Gastrointestinal

    • Genitourinary

    • Joints

  • Patterns of bleeding

    • Recent onset or lifelong

    • Frequency and severity

    • Spontaneous or following injury

  • Challenges to hemostasis

    • Dental extraction

    • Operative or other invasive procedures

    • Medications

  • Associated diseases

    • Uremia: most commonly associated with platelet dysfunction

    • Liver disease: most commonly associated with coagulation factor deficits

    • Infection: could be associated with either platelet or coagulation deficits

    • Malignant neoplasm: could be associated with either platelet or coagulation deficits

  • Previous transfusion history

  • Family history

Physical Examination

  • Vital signs

  • Skin: Nature of bleeding, signs of liver disease, petechial, purpura and distribution of skin abnormalities.

  • Mucosa: Oral or nasal, epistaxis

  • Lymphadenopathy

  • Abdomen: Liver size and shape, splenomegaly

  • Joints: Signs of previous bleeding (limited joint movement, pain mimicking osteoarthritis)

  • Other sites of blood loss: Pelvic, rectal, urinary tract, intramuscular or deep soft tissue

Platelet disorders are usually manifested as acquired petechiae, purpura, or mucosal bleeding, and are more common in women. Platelet abnormalities can be caused by congenital disorders, though most are related to acquired conditions. The bleeding source is usually a capillary with resultant cutaneous and mucosal petechiae or ecchymosis. Epistaxis, menorrhagia, and gastrointestinal bleeding are common initial symptoms. The bleeding is generally mild and may occur immediately after surgery or dental extractions. The presence of petechiae or purpura may be noted on examination, and superficial ecchymoses may develop around venipuncture sites. The purpura associated with platelet disorders is typically asymptomatic and not palpable. This is in contrast to purpura associated with vasculitis, which can burn or itch and is palpable. Vascular disorders such as vasculitis are associated with signs and symptoms similar to those of thrombocytopenic states. Inherited vascular disorders are rare, and acquired forms are usually associated with connective tissue changes or endothelial damage.

Coagulation issues may be congenital in nature, characterized by delayed deep muscle or joint bleeding, and occur more often in men. Clinically significant coagulation disorders have a number of characteristic features that help differentiate them from platelet disorders ( Box 111.5 ).

BOX 111.5
Features of Coagulation Disorders That Differentiate From Platelet Disorders

  • The bleeding source is often an intramuscular or deep soft tissue hematoma from small arterioles.

  • The congenital form of the disease occurs predominantly in men, often via sex-linked inheritance.

  • Bleeding may occur after surgery or trauma but may be delayed in onset up to 72 hours.

  • Epistaxis, menorrhagia, and gastrointestinal sources of bleeding are rare, whereas hematuria or hemarthrosis are common in severe cases.

  • The bleeding time is normal except in patients with von Willebrand disease (vWD).

Differential Diagnosis

The differential of platelet disorders is listed in Box 111.6 . The differential of vascular disorders is listed in Box 111.7 . The differential for coagulation disorders is listed in Box 111.8 .

BOX 111.6
Differential Diagnosis of Platelet Disorders

Decreased Platelet Count (Thrombocytopenia)

  • Decreased production

    • Decreased megakaryocytes secondary to drugs, toxins, or infection

    • Normal megakaryocytes with megaloblastic hematopoiesis or hereditary origin

    • Platelet pooling and splenic sequestration

  • Increased destruction

    • Immunologic

      • Related to collagen vascular disease, lymphoma, leukemia

      • Drug related

      • Infection

      • Post-transfusion

      • Immune thrombocytopenia

    • Mechanical

      • Disseminated intravascular coagulation (DIC)

      • Thrombotic thrombocytopenic purpura (TTP)

      • Hemolytic-uremic syndrome (HUS)

      • Hemolysis elevated liver function tests & low platelets (HELLP) syndrome related to pregnancy

    • Vasculitis

  • Dilutional secondary to massive blood transfusion

Platelet Dysfunction (Thrombocytopathy)

  • Adhesion defects such as von Willebrand disease (vWD)

  • Release defects: Acquired or drug related

  • Aggregation defects, such as in thrombasthenia

Elevated Platelet Count (Thrombocytosis)

  • Autonomous (primary thrombocythemia)

  • Reactive (secondary thrombocythemia)

  • Iron deficiency

  • Infection or inflammation

  • Trauma

  • Nonhematologic malignant disease

  • Post-splenectomy

  • Rebound from alcohol, cytotoxic drug therapy, folate or vitamin B 12 deficiency

BOX 111.7
Differential Diagnosis of Vascular Disorders

Inherited

  • Disorders of connective tissue

    • Pseudoxanthoma elasticum

    • Ehlers-Danlos syndrome

    • Osteogenesis imperfecta

  • Disorders of blood vessels

    • Hemorrhagic telangiectasia

Acquired

  • Scurvy (vitamin C deficiency)

  • Simple or senile purpura

  • Purpura secondary to steroid use

  • Vascular damage

    • Infection (meningococcemia)

    • Hemolytic-uremic syndrome (HUS)

    • Hypoxemia

    • Thrombotic thrombocytopenic purpura (TTP)

    • Dysproteinemic purpura

BOX 111.8
Differential Diagnosis of Coagulation Disorders

Inherited

  • Von Willebrand disease

  • Hemophilia A (factor VIII) or hemophilia B (factor IX)

  • Factor XIII, factor XI, factor X, factor VII, factor V or factor II deficiency

  • Afibrinogenemia/hypofibrinogenemia

Acquired

  • Medication

  • Snake bite (venom-induced consumptive coagulopathy)

  • Liver disease

  • Disseminated intravascular coagulation (DIC)

  • Autoimmune disorders (including autoantibodies towards factors such as fibrinogen)

  • Acquired factor inhibitors, from treatment of congenital disorder such as hemophilia, or malignancy

Diagnostic Testing

A definitive diagnosis is dependent on laboratory evaluation. Tests pertinent to the ED setting are discussed in the following sections and are listed in Box 111.9 .

BOX 111.9
Diagnostic Hemostasis Tests
BUN, Blood urea nitrogen; EDTA, ethylenediaminetetraacetic acid.

  • Complete blood count and smear (EDTA—purple top)

  • Platelet count (EDTA—purple top)

  • Bleeding time

  • Prothrombin time/International normalized ratio (PT/INR; citrate—blue top)

  • Partial thromboplastin time (PTT; citrate—blue top)

  • Other coagulation studies: Fibrinogen level, anti-factor Xa assay, thrombin time, clot solubility, factor levels, inhibitor screens

  • As necessary: Serum electrolyte levels; serum glucose, BUN, and creatinine concentrations; type and crossmatch

Complete Blood Count and Blood Smear

The complete blood count can, in some cases, assess the degree of anemia associated with a bleeding episode. Reductions in hemoglobin and hematocrit often lag behind the actual loss of RBCs in acute hemorrhage owing to the time necessary for equilibration. The peripheral blood smear may demonstrate schistocytes or fragmented RBCs in microangiopathic hemolytic anemias, such as TTP or DIC. Teardrop-shaped or nucleated RBCs may reflect myelophthisic disease where hematopoietic bone marrow is infiltrated and replaced by fibrosis, tumors, or granulomas. Characteristic white blood cell morphologies are seen with thrombocytopenia associated with infectious mononucleosis (e.g., increased WBC cytoplasm and nucleoli in the nuclei), folate or vitamin B 12 deficiency (e.g., hypersegmented neutrophils), or leukemia (e.g., immature WBCs, hairy cell lymphocytes, and myeloblasts with Auer rods).

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