PT/APTT
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PT
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APTT
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| Factors Affected
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I, II, V, VII, X
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All except VII - Congenital def. of VIII, IX, or XI - VWF disease → low VIII
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| Pathways Affected
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Extrinsic and common
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Intrinsic and common
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| Drugs Monitored
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Coumadin (warfarin)
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Heparin (unfractionated)
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| Conditions
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- Specific factor antibodies
- Non-specific inhibitors
- Coagulation factor deficiencies
- Unexplained bleeding/bruising
- Recurrent miscarriages
- Disseminated intravascular coagulation (DIC)
- Recurrent thrombosis
- Prior to surgery when increased risk of blood loss or history of bleeding
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| Interfering Factors
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- Drugs (antihistamines, ascorbic acid - Vitamin C, chlorpromazine, heparin, salicylates)
- Incorrect anticoagulant
- Hematocrit (increased/decreased)
- Sample from heparin lock or heparinized catheter
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| RI
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- PT: 9.5-13.5 s
- INR: 0.9 - 1.2
- INR (warfarin): 2.0-3.0
- INR (warfarin + cardiac condition OR LA): 2.5-3.5
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- APTT: 25-35s
- APTT (heparin): 1.5-2.5x mean)
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Reflex/Follow-up Testing
| Test (RI)
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Info
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Ordered When
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| Thrombin Time (15-20s)
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Assesses deficiencies or dysfunction of fibrinogen (Factor I) or thrombin (Factor II) inhibitor Less fibrinogen available → longer clot time
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- Bleeding or thrombotic episodes
- Recurrent miscarriages
- BOTH PT and APTT unexpectedly prolonged
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- Congenital fibrinogen deficiency
- Heparin therapy
- Direct thrombin inhibitor therapy
- Contamination
- Presences of thrombin or fibrinogen inhibitors (rare)
- Acquired hypofibrinogenemia from liver disease or massive hemorrhage
- Abnormal fibrinolysis
- Increased products of clot breakdown interfering with fibrin polymerization (e.g., DIC)
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| Fibrinogen
(2.2-5.0 g/L)
(Critical: <1.0g/L with increased PT, APTT, TT)
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Modified TT assay that estimates concentration of functional fibrinogen Clotting time correlates with active fibrinogen
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- Acquired hypofibrinogenemia
- Assess inflammatory conditions
- Recurrent miscarriages
- Suspected congenital fibrinogen deficiency or abnormality
- BOTH PT and APTT unexpectedly prolonged
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| D-Dimer
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Measures fibrin clot breakdown products from plasmin Elevated D-dimer alone is non-specific except in VTE - Can be associated with a variety of diseases or inflammatory states
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- Deep vein thrombosis
- Pulmonary embolism
- Recent surgery/trauma
- Some cancers
- Acute/chronic infections or inflammatory diseases
- DIC
- Very heavy menstruation
- Normal pregnancy (high levels associated with complications)
- Healthy elderly patient Negative result can be used to exclude venousthromboembolism (VTE) in some populations
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| Mixing Studies
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| Inhibitor Testing
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| Factor Assays
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Abnormal Results
If PT/INR and APTT both prolonged
- Multiple factors in intrinsic and extrinsic pathways affected OR single factor deficiency in common pathway (I, II, V, or X [I if severe])
- Congenital:
- Single factor deficiency for factor I, II, V, or X
- Acquired:
- Multiple factor deficiency in intrinsic AND extrinsic pathways
- Severe liver disease
- Severe Vitamin K deficiency
- DIC
- Specific inhibitor directed to common pathway factor
- Hypofibrinogenemia/dysfibrinogenemia
- Massive hemmorage
- Congenital
- Fibrinolysis
If PT/INR is prolonged, but APTT is normal
- Probably related to factor VII
- Congenital single factor VII deficiency
- Acquired
- Early liver disease
- Early vitamin K deficiency
- Early coumadin therapy or initial dose
- Specific inhibitor to VII (rare)
If APTT is prolonged, but PT/INR is normal
- Probably related to intrinsic pathway factors VIII, IX, XI, or contact factors
- Congenital
- Single factor deficiency of VIII, IX, XI with bleeding (hemophilia A, B, or C respectively)
- VWD (can lead to factor VIII deficiency)
- Deficiency of factor XII, pre-K, HMWK (contact factors)
- Prolongs APTT but doesn’t result in clinically significant bleeding
- Acquired
- Non-specific inhibitor (e.g., antiphospholipid antibodies)
- Lupus anticoagulant in SLE patients
- Specific inhibitor against intrinsic factors
- Hemophilia patients may develop anti-FVIII or IX due to treatment
- Acquired hemophilia or acquired VWD
- Heparin therapy
Causes of Abnormal Results + Followup Testing
| Test Affected
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Cause
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Disease States
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Symptoms/Patient History
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Pathways Affected
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Followup Testing
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| BOTH PT and APTT
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Single factor deficiency for I, II, V, or X
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| Multiple factor deficiency in intrinsic AND extrinsic pathways
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Severe liver disease
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Jaundice, abdominal pain or tenderness
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- CBC (platelet count)
- RBC morphology (macrocytes and targets)
- Thrombin time/fibrinogen
- D-Dimer
- Factor V assay (decreased in liver disease but not Vit K deficiency)
- Factor VII assay (most sensitive factor)
- Mixing studies
- Liver enzyme panel
- Total and indirect bilirubin
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| Severe Vitamin K deficiency
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| Disseminated intravascular coagulation
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| Specific inhibitor to common pathway factor
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| Hypofibrinogenemia/dysfibrinogenemia
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| PT only
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Factor VIII deficiency
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Congenital single factor VII deficiency
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| Early liver disease
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| Early Vitamin K deficiency
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| Early coumadin therapy/initial dose
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| Specific inhibitor to VIII (rare)
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| APTT only
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VWF disease
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- Young patient of any gender
- Mucocutaneous bleeding (nosebleeds, menorrhagia, etc.)
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Factor VIII
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- CBC (PLT count to rule out thrombocytopenia)
- PT/APTT (to rule out other coagulation issues)
- VWF:Ag quantitative analysis immunoassay
- VWF:RCo Ristocetin co-factor qualitative analysis
- Factor VIII activity assay (FVIII:C)
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Hemophilia A, B, or C (single factor deficiency)
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- Male patient
- Anatomic soft tissue bleeding (deep bleeding in muscles, joints, organs)
- Wound oozing after trauma or surgery
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- Factor VIII (Hemophilia A - 85%)
- Factor IX (Hemophilia B - 14%)
- Factor XI or other factors (Hemophilia C - 1%)
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- Mixing studies (should be corrected)
- Factor assays (decrease in specific factor relevant to Hemophilia)
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Other congenital factor deficiencies
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Non-specific inhibitor
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Specific inhibitor against intrinsic factors
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Heparin therapy
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Investigating Abnormal Results
- Check specimen integrity and HCT >55% (recollect and/or dilute)
- Check patient history for any conditions affecting coagulation. If present, report results:
- Anticoagulant therapy: warfarin/coumadin, heparin, direct oral anticoagulants (DOACs)
- Liver disease (early: PT, late: both PT/APTT)
- Vitamin K deficiency
- Known factor deficiency (single or multiple)
- Look for other causes and perform reflex testing
- Decreased fibrinogen → Thrombin time or fibrinogen assay
- Specific single or multiple factor deficiency
- Inhibitor or antibody to factors
- Inhibitor or antibody interfering with test
