Pathology of Hemostasis Disorders

Question 1

thrombocytopenia - defined

Answer 1

*defined by platelets < 150,000
*spontaneous bleeding occurs at platelets < 20,000
-usually involves small vessels of skin, mucous membranes, GI/GU tracts
-intracranial bleeding can be serious!

Question 2

causes of thrombocytopenia

Answer 2

1. decreased platelet production = bone marrow problems (aplastic anemia, MDS, vitamin deficiency, tumors)
2. decreased platelet survival
   a. immunologic (circulating anti-platelet antibodies to GpIIb/IIIa or GpIB) - ex. ITP, HIV, drugs
   b. mechanical destruction/consumption - ex. MAHA, prosthetic heart valves
3. sequestration
4. dilutional

Question 3

thrombocytosis - defined

Answer 3

*defined by platelets > 350K
*complications:
-thrombotic episodes, due to increased number of active platelets
-bleeding episodes, as platelet function may also be defective

Question 4

causes of thrombocytosis

Answer 4

1. primary causes: myeloproliferative neoplasms (essential thrombocytosis, CML, PV, PMF)
2. secondary/reactive causes: infections, iron deficiency, inflammatory disorders, etc

Question 5

immune thrombocytopenic purpura (ITP) - pathogenesis

Answer 5

*antiplatelet antibodies to GpIIb/IIIa or GpI/IX:
-coat platelets, which are selectively removed from circulation by the spleen

Question 6

immune thrombocytopenic purpura (ITP) - causes

Answer 6

*may be secondary or primary (idiopathic)
1. acute:
-children
-self-limiting
-post acute viral infection
2. chronic:
-adults
-autoimmune syndromes, infections, drugs, HIV

Question 7

immune thrombocytopenic purpura (ITP) - diagnosis

Answer 7

*isolated thrombocytopenia in otherwise healthy pt (no other cell counts low)
*NORMAL PT, aPTT
*normal/increased numbers of megakaryocytes in bone marrow

*RULE OUT: no known exposure to thrombocytopenic agents

Question 8

ddx for: normal PT, elevated aPTT, normal platelets

Answer 8

*VIII, IX, XI deficiencies (deficiencies of INTRINSIC pathway)
*VWD (von willebrand disease)
*heparin

Question 9

ddx for: elevated PT, elevated aPTT, normal platelets

Answer 9

liver disease

Question 10

ddx for: elevated PT, elevated aPTT, decreased platelets

Answer 10

DIC (fibrinogen also low)

Question 11

ddx for: normal PT, normal aPTT, decreased platelets

Answer 11

*hypersplenism
*platelet destruction/production (ITP, TTP, HUS)

Question 12

ddx for: normal PT, normal aPTT, increased platelets

Answer 12

reactive vs. myeloproliferative disorder

Question 13

D-dimer lab test

Answer 13

*specific plasmin-mediated breakdown product of cross-linked fibrin
*normal < 200 ng/mL
*useful for:
-DIC (level usually very elevated)
-DVT, post-op, acutely ill level elevated, not as high as seen in DIC

Question 14

RBC fragmentation syndromes

Answer 14

1. mechanical/vascular hemolysis: direct mechanical trauma from hemodynamic defect or extreme turbulence
   -prosthetic heart valves, vascular malformations, malignant hypertension, severe burns, “March hemoglobinuria”
2. microangiopathic hemolytic anemias (MAHA): endothelial damage in microvasculature
   -DIC, TTP, HUS

Question 15

microangiopathic hemolytic anemias (MAHA)

Answer 15

*RBCs are damaged when passing through obstructed or narrowed vessels
*causes intravascular hemolysis
*examples:
1. disseminated intravascular coagulation (DIC)
2. thrombotic thrombocytopenic purpura (TTP)
3. hemolytic uremic syndrome (HUS)

Question 16

disseminated intravascular coagulation (DIC) - overview

Answer 16

*a secondary condition in which microthrombi develop throughout the bloodstream, blocking small blood vessels and depleting platelets and clotting factors needed to control bleeding
*widespread clotting factor activation → thromboembolic state with excessive clotting factor consumption → increased thrombosess, increased hemorrhages

Question 17

disseminated intravascular coagulation (DIC) - pathogenesis

Answer 17

*simultaneous systemic activation of:

1. coagulation system:
   -widespread expression of tissue factor (TF)
   ~intravascular thrombus formation (compromising blood supply to various organs)
   ~exhaustion of platelets and coagulation factors, resulting in hemorrhage
2. fibrinolytic system:
   -plasmin degrades fibrinogen and fibrin, producing fibrin degradation products, exacerbating bleeding

Question 18

disorders associated with disseminated intravascular coagulation (DIC)

Answer 18

*malignancies (solid tumor, hematologic)
*obstetric emergencies (amniotic fluid embolism, abruptio placentae)
*organ destruction (severe pancreatitis, severe hepatic failure)
*sepsis/severe infection
*severe toxic or immunologic reactions
*trauma
*vascular abnormalities

Question 19

disseminated intravascular coagulation (DIC) - common triggers

Answer 19

1. massive tissue destruction
2. sepsis
3. endothelial cell injury

note - all three of these cause mass release of tissue factor

Question 20

disseminated intravascular coagulation (DIC) - clinical features

Answer 20

*usually severe bleeding:
-petechiae/ecchymoses of skin/mucous membranes
-shock
*signs of the underlying disease are usually present
*organ(s) involved with accompanying clinical signs must also be taken into consideration

Question 21

disseminated intravascular coagulation (DIC) - LABS

Answer 21

*increased PT
*increased aPTT
*decreased platelets (thrombocytopenia)
*decreased fibrinogen; increased D-dimer
*microangiopathic hemolytic anemia with SCHISTOCYTES on peripheral smear

Question 22

thrombotic thrombocytopenic purpura (TTP) - clinical pentad

Answer 22

*microangiopathic hemolytic anemia (decreased Hb, schistocytes, and increased LDH)
*NEUROLOGIC abnormalities
*renal insufficiency (decreased creatinine)
*fever
*thrombocytopenia

Question 23

thrombotic thrombocytopenic purpura (TTP) - pathophysiology

Answer 23

inhibition or deficiency of ADAMTS13 (a vWF metalloprotease) → decreased degradation of vWF multimers → increased large vWF multimers → increased platelet adhesion and aggregation (microthrombi formation)

Question 24

thrombotic thrombocytopenic purpura (TTP) - lab diagnosis

Answer 24

*deficiency of vWF metalloprotease ADAMTS13 (results in accumulation of very-high-molecular-weight multimers of vWF, promoting platelet aggregation)
*consumptive thrombocytopenia (LOW PLATELETS)
*NORMAL PT and PTT
*MAHA with schistocytes in blood smears (low Hb, high LDH)

Question 25

hemolytic uremic syndrome (HUS) - clinical features

Answer 25

*microangiopathic hemolytic anemia (decreased Hb, schistocytes, increased LDH) *thrombocytopenia *renal insufficiency ***bloody diarrhea**

Question 26

hemolytic uremic syndrome (HUS) - pathogenesis

Answer 26

*predominantly caused by **Shiga toxin-producing E. coli (STEC) infection (serotype 0157:H7)**, which causes profound endothelial dysfunction

Question 27

hemolytic uremic syndrome (HUS) - lab diagnosis

Answer 27

***E. coli 0157:H7 infectious gastroenteritis:** -elaborates shiga-like toxin absorbed by GI tract and binds to endothelial cells, initiating platelet activation *consumptive thrombocytopenia **(LOW PLATELETS) *NORMAL PT and PTT** *MAHA with schistocytes in blood smears (low Hb, high LDH)

Question 28

what can help you distinguish TTP from HUS?

Answer 28

1. HUS = bloody diarrhea; TTP = neuro symptoms 2. HUS = E. coli 0157:H7; TTP = ADAMTS13 deficiency

Question 29

von Willebrand Factor (vWF) - functions

Answer 29

1. binds to GpIb receptor on platelets → adhesion to damaged epithelium 2. carrier protein for VIII (stabilized VIII, increasing serum half life)

Question 30

von Willebrand Disease (VWD) - epidemiology

Answer 30

*most common bleeding disorder *affects 1% of general population *autosomal dominant OR recessive: -multiple genetic mutations -results in either a QUANTITATIVE or QUALITATIVE deficiency of vWF

Question 31

von Willebrand Disease (VWD) - overview

Answer 31

*INTRINSIC pathway coagulation defect: **decreased quantity/function of vWF → ELEVATED PTT (vWF carries/protects factor VIII)** *defect in platelet plug formation → defect in platelet-to-vWF adhesion *commonly presents with menorrhagia or epistaxis

Question 32

von Willebrand Disease (VWD) - diagnostic approach

Answer 32

*hematologic evaluation of peripheral blood *screening for hemostasis (platelet count, PT, aPTT, etc) *VWD panel (esoteric testing): -decreased factor VIII activity -decreased vWF antigen -decreased ristocetin cofactor activity

Question 33

Factor VIII deficiency (Hemophilia A) - labs

Answer 33

***prolonged PTT, normal PT** *factor VIII-specific assays are required

Question 34

acquired coagulopathies

Answer 34

1. liver disease: -liver is the major site of clotting factor synthesis -hepatitis/cirrhosis -results in bleeding diathesis 2. Vitamin K deficiency -biliary obstruction, malabsorption syndromes, nutritional deficiencies -drugs affecting gut flora -results in bleeding diathesis 3. DIC -tissue factor express -results in purpuric manifestations

Question 35

Factor V Leiden - epidemiology

Answer 35

*most common inherited **thrombotic** disorder (results in a **hypercoagulable state)** *accounts for 20-50% of thrombotic disorders *autosomal dominant: **-point substitution resulting in Arg506 -> Gln -mutation in Factor V renders it resistant to proteolysis by activated Protein C**

Question 36

Factor V Leiden - clinical features

Answer 36

*recurrent venous thromboembolism, may be asymptomatic

Question 37

Factor V Leiden - diagnosis

Answer 37

DNA mutational analysis

Question 38

Factor V Leiden - treatment

Answer 38

*prophylactic anticoagulation (warfarin)

Question 39

ddx for: increased PT, normal aPTT, normal platelets

Answer 39

*VII, X, V deficiencies *Vitamin K deficiency