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Time Completed: 02:25:57

Final Score 83%

149
31

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Pathology

Haematology

Question 167 of 180

Which of the following is NOT a recognised risk factor for venous thrombosis:

Answer:

Approximately one-third of patients who suffer DVT or PE have an identifiable heritable risk factor, although additional risk factors are usually present when they develop the thrombosis. The history of a spontaneous DVT in a close relative increases an individual's risk of DVT even if no known genetic predisposition can be identified.

There are three main components important in venous thrombus formation described by Virchow's triad:

  • Decreased rate of blood flow (e.g. by venous insufficiency, prolonged immobility or varicose veins)
  • Hypercoagulability of blood (e.g. by hyperviscosity or thrombophilia disorders)
  • Vessel wall damage (e.g. by sepsis, indwelling venous catheter or by previous thrombosis)

Risk Factors for Venous Thrombosis

  • Inherited risk factors:
    • Factor V Leiden (most common)
    • Prothrombin variant
    • Protein C or protein S deficiency
    • Antithrombin deficiency
  • Acquired risk factors include:
    • Lupus anticoagulant
    • Oestrogen therapy (OCP and HRT)
    • Heparin-induced thrombocytopaenia
    • Pregnancy and puerperium
    • Surgery (especially abdominal, hip and knee surgery)
    • Major trauma
    • Malignancy (especially of the ovary, brain and pancreas)
    • Myeloproliferative disorders
    • Acutely ill hospitalised medical patients
    • Hyperviscosity, polycythaemia
    • Stroke
    • Pelvic obstruction
    • Nephrotic syndrome
    • Dehydration
    • Varicose veins
    • Previous venous thrombosis
    • Age
    • Obesity
    • Paroxysmal nocturnal haemoglobinuria
    • Behcet's disease

Approximately one-third of patients who suffer DVT or PE have an identifiable heritable risk factor, although additional risk factors are usually present when they develop the thrombosis. The history of a spontaneous DVT in a close relative increases an individual's risk of DVT even if no known genetic predisposition can be identified.

Factor V Leiden

Factor V Leiden gene mutation is the most common inherited cause of an increased risk of venous thrombosis. Activated protein C normally breaks down activated factor V and so should slow the clotting reaction and prolong the APTT, but a mutation in the factor V gene makes factor V less susceptible to cleavage by activated protein C, resulting in increased levels of activated factor V.

Heterozygotes for factor V Leiden are at an approximately five- to eight- fold increased risk of venous thrombosis compared to the general population (but only 10% of carriers will develop thrombosis in their lifetime). Homozygotes have a 30 - 140-fold increased risk. The incidence of factor V Leiden in patients with venous thrombosis is approximately 20 - 40%. It does not increase the risk of arterial thrombosis.

Diagnosis of Venous Thrombosis

Deep Vein Thrombosis (DVT):

  • Clinical Suspicion
    • DVT is suspected in patients with a painful swollen limb
    • Signs may include unilateral thigh or calf swelling or tenderness, changes to skin colour, and venous distension
  • Plasma D-dimer concentration
    • The concentration of fibrin degradation products (FDPs) is raised when there is a fresh thrombosis; this may be used to exclude diagnosis when used in conjunction with a clinical probability tool
  • Compression ultrasound
    • This is a reliable and practical method for patients with suspected DVT in the legs and other sites

Pulmonary Embolism (PE):

  • Clinical Suspicion
    • PE is suspected in patients with shortness of breath and pleuritic chest pain
    • Signs may include tachycardia, tachypnoea, hypoxia and pyrexia
  • Chest x-ray
    • This is often normal but may show evidence of pulmonary infarction or pleural effusion
  • Electrocardiogram
    • This may show right heart strain in severe cases
  • Plasma D-dimer concentration
    • This may be used to exclude diagnosis when used in conjunction with a clinical probability tool
  • Ventilation perfusion (VQ) scintigraphy
    • This detects areas of the lungs being ventilated but not perfused
  • Computed tomography pulmonary angiography (CTPA)
    • Fine slices of the lung are scanned by spiral CT to identify filling defects in the pulmonary arteries

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  • Biochemistry
  • Blood Gases
  • Haematology
Biochemistry Normal Value
Sodium 135 – 145 mmol/l
Potassium 3.0 – 4.5 mmol/l
Urea 2.5 – 7.5 mmol/l
Glucose 3.5 – 5.0 mmol/l
Creatinine 35 – 135 μmol/l
Alanine Aminotransferase (ALT) 5 – 35 U/l
Gamma-glutamyl Transferase (GGT) < 65 U/l
Alkaline Phosphatase (ALP) 30 – 135 U/l
Aspartate Aminotransferase (AST) < 40 U/l
Total Protein 60 – 80 g/l
Albumin 35 – 50 g/l
Globulin 2.4 – 3.5 g/dl
Amylase < 70 U/l
Total Bilirubin 3 – 17 μmol/l
Calcium 2.1 – 2.5 mmol/l
Chloride 95 – 105 mmol/l
Phosphate 0.8 – 1.4 mmol/l
Haematology Normal Value
Haemoglobin 11.5 – 16.6 g/dl
White Blood Cells 4.0 – 11.0 x 109/l
Platelets 150 – 450 x 109/l
MCV 80 – 96 fl
MCHC 32 – 36 g/dl
Neutrophils 2.0 – 7.5 x 109/l
Lymphocytes 1.5 – 4.0 x 109/l
Monocytes 0.3 – 1.0 x 109/l
Eosinophils 0.1 – 0.5 x 109/l
Basophils < 0.2 x 109/l
Reticulocytes < 2%
Haematocrit 0.35 – 0.49
Red Cell Distribution Width 11 – 15%
Blood Gases Normal Value
pH 7.35 – 7.45
pO2 11 – 14 kPa
pCO2 4.5 – 6.0 kPa
Base Excess -2 – +2 mmol/l
Bicarbonate 24 – 30 mmol/l
Lactate < 2 mmol/l

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