Week 6 Coagulation Lecture 4 - Inhibition of Haemostasis Flashcards
Coagulation Pathway Revision
The most crucial step is the generation of thrombin
Thrombin generation is initiated when damage to a vessel wall exposes the blood to tissue factor (TF) in the sub-endothelium
TF forms a complex with FVIIa and activates FX
Together, FVa & FXa form the prothrombinase complex, which then cleaves a small amount of prothrombin (FII) to thrombin (FIIa)
This small amount of thrombin activates platelets, FV, FVIII and FXI, feeding back into the cycle to increase thrombin formation
Factor IXa, previously activated by either TF-VIIa or by FXIa on the platelet surface, and FVIIIa in the presence of calcium, complex on the platelet surface to form the platelet tenase complex
Platelet tenase activates more FX, which with FVa, generates a thrombin burst
It is this burst of thrombin rather than the initial thrombin activation that is crucial for the formation of a stable haemostatic plug
Physiological Inhibitors of Coagulation
Several mechanisms:
- tissue factor pathway inhibitor (TFPI)
- antithrombins
- protein C/S system
- protein Z/ZPI system
Act upon factors within the coagulation cascade
Typically act to inactivate factors that have been activated
Tissue Factor Pathway Inhibitor (TFPI)
Major inhibitor of blood coagulation
Produced by predominantly by endothelial cells & megakaryocytes
There are two isoforms resulting from alternative splicing
- TFPIα, TFPIβ
- both present in endothelial cells
- platelets only have TFPIα
TFPIα contains three Kunitz domains (K1, K2 and K3) followed by a positively charged C-terminal tail
TFPIβ which consist of K1 and K2 followed by a unique C-terminus encoding for a glycosyl-phosphatidylinositol (GPI) anchor
The K1 and K2 domains of TFPIα bind & inhibit FVIIa
The K1 and K2 domains of TFPIβ bind & inhibit FXa
The K3 domain is known to bind protein S => Protein S enhances FXa inhibition by TFPIα
Antithrombin-Glycosaminoglycan Pathway
Antithrombin is:
- produced by the liver
- not Vitamin K dependent
- serine protease inhibitor (SERPIN)
- important physiological inhibitor of thrombin
- inhibits FIIa, FXa (& also FIXa, FVIIa)
Importantly AT when binds to heparin sulphate
- activity increase x1000
- prostacyclin (PGI2) synthesis, vasodilation,
- inhibits platelet aggregation
Protein C/S System - Protein C
Circulating Vitamin K dependent protein when activated significantly prolongs the clotting time of normal plasma
Activated via thrombin (& thrombomodulin)
Endothelial Protein C receptor (EPCR) binds Protein C & presents to thrombin
Results in activated Protein C (APC)
Activated Protein C inhibits FVa & FVIIIa
Cofactors: Protein S, phospholipid
Limited by protein C inhibitor, α2-macroglobulin, α1- antitrypsin
Protein C/S System - Protein S
Vitamin K dependent glycoprotein
Produced by liver & endothelial cells
Exists in plasma as free & bound forms (to C4b-binding protein)
Free form only has anticoagulant activity
Co-factor to APC in FVa & FVIIIa inactivation
Also has anticoagulant activity independent of APC on FVaFXa complex
Protein Z/Z Dependent Protease Inhibitor
Protein Z dependent protease inhibitor (ZPI) =>
inhibits FXa
Requires presence of Protein Z & calcium ions
Protein Z is a vitamin K dependent glycoprotein that acts as a cofactor of ZPI
ZPI also inhibits FIXa, FXIa independent of Protein Z
Disorders of Anticoagulants
Deficiency of anticoagulant typically predisposes to venous thrombosis
Typically comprise 5-10% of patients with clinical venous thromboembolism (VTE)
Include
- AT deficiency
- TFPIα deficiency
- APC resistance
- protein C deficiency
- protein S deficiency
Antithrombin Deficiency May Result From…
- Decreased production
- liver cirrhosis - Increased loss
- nephrotic syndrome
- protein losing enteropathy - Enhanced consumption
- sepsis
- burns
- disseminated intravascular coagulation (DIC)
- prolonged unfractionated heparin therapy
Pathological Inhibitors of Coagulation
Substances that inhibit the normal functioning of coagulation cascade
Result in haemorrhagic diathesis
Include:
- auto-antibodies to coagulation cascade factors
- antiphospholipid syndrome
Haemophiliac vs Non-Haemophiliac
Haemophiliac
- ‘inhibitors’ = antibodies to coagulation factors
- e.g. Haemophilia A; inhibitors form in response to transfusion FVIII concentrate
Non-haemophiliacs
- ‘acquired’ haemophilia
- e.g. formation antibodies to FVIII without known cause
- initially recognised with ↑ aPTT
Definition of Inhibitors
An inhibitor is a high affinity IgG antibody that specifically neutralises the procoagulant activity of the relevant clotting factor
High responders = >5 (BU/mL)
Low responders = <5 (BU/mL)
Principle of the Bethesda Titre
FVIII inhibitors may quantified by mixing plasma with a known amount of FVIII
Incubated @ 37°C for 2h
Amount of inhibitor calculated as the difference from control mixture containing pooled plasma & buffer
1 Bethesda unit = inhibitor that will inactivate half the factor present in mixture of equal volumes of patient plasma & pooled normal plasma after 2h of incubation
Acquired Haemophilia A (AHA)
Caused by autoantibodies against FVIII
Clinically, AHA is similar to severe haemophilia A with an increased risk of spontaneous bleeds, but the bleeding is usually mucocutaneous, soft tissue or gastrointestinal
Aetiology:
- 50% of cases have FVIII autoantibodies
- the remaining cases may be associated with postpartum period, autoimmune diseases, cancers, infections
Diagnosis of AHA
Identified ↑ aPTT
Mixing test (rule in inhibitor, rule out deficiency)
Test for anti-phospholipid antibodies
Confirm with Bethesda Assay for anti-FVIII antibodies
