62878
Haemostasis (part 1:
primary haemostasis)
- Introduction
- The pysiological
response to blood
vessel damage that
acts to minimise
blood loss
- Balance between protecting from
haemorrhage and thrombosis
- Primary haemostasis = platelet plug formation
- Secondary haemostasis = fibrin clot formation
- General
mechanism
- Blood vessel injury
- Platelet aggregation
- Platelet
activation
- +
- +
- Platelet
activation
- (Neural) vessel constriction
- Reduced
blood flow
- Stable
haemostatic
plug
- Stable
haemostatic
plug
- Reduced
blood flow
- (Tissue factor) coagulation cascade
- Fibrin formation
- Fibrin formation
- Platelet aggregation
- Blood vessel injury
- The pysiological
response to blood
vessel damage that
acts to minimise
blood loss
- Primary haemostasis players
- Endothelium
- Normally the endothelium prevents thrombus
formation by actively exhibiting antiplatlet,
anticoagulant and profibrinolytic properties
- Antiplatelet properties
- The endothelium serves as a barrier
between the highly pro-thrombotic
ECM and the platelets in circulation
- Secrete NO (nitric oxide) and
prostaglandin I-2 (PGI2) which
promotes vasodilation and
inhibits the activation of platelets
- Also expresses adenylate
diphosphatase (ADPase) which
degrades circulating ADP (an
activator of platelets)
- The endothelium serves as a barrier
between the highly pro-thrombotic
ECM and the platelets in circulation
- Anticoagulative
- The endothelial cells
feature membrane-bound
thrombomodulin
- Thrombomodulin binds to thrombin (converting it
from a pro-thrombotic to anti-thrombotic protein)
- This activates protein C (an inhibitor of the coagulation cascade)
- Protein C (with protein S) inhibits coagulation factors Va and VIIIa
- Protein C (with protein S) inhibits coagulation factors Va and VIIIa
- This activates protein C (an inhibitor of the coagulation cascade)
- Thrombomodulin binds to thrombin (converting it
from a pro-thrombotic to anti-thrombotic protein)
- Endothelial membrane-bound
heparin-like molecules act as cofactors
- Bind as cofactors to antithrombin(III)
- Activated antithrombin(III)
- Inactivates
thrombin
- Inactivates factors IXa and Xa
- Inactivates
thrombin
- Activated antithrombin(III)
- Bind as cofactors to antithrombin(III)
- The endothelial cells
feature membrane-bound
thrombomodulin
- Profibrinolytic
- Endothelial cells produce t-PA
(tissue plasminogen activator)
- t-PA cleaves plasminogen into plasmin
(which degrades fibrin - degrades thrombi)
- t-PA cleaves plasminogen into plasmin
(which degrades fibrin - degrades thrombi)
- Endothelial cells produce t-PA
(tissue plasminogen activator)
- Antiplatelet properties
- Prothrombotic
qualities
(following injury)
- Loss of endothelium reveals ECM
collagen-bound vWF -> platelets biond
vWF (via the platelet glycoprotein GPIb)
- Procoagulative
- In response to inflammatory cytokines (TNF,
IL-1) endothelial cells prodcue tissue factor
- Tissue factor activates the
extrinsic coagulation cascade
- Tissue factor activates the
extrinsic coagulation cascade
- In response to inflammatory cytokines (TNF,
IL-1) endothelial cells prodcue tissue factor
- Anti-fibrinolytic
- Under the right circumstances (injury
etc.) endothelial cells produce inhibitors
of plasminogen activator (PAI's)
- Prevents plasmin-mediated fibrinolysis
- Prevents plasmin-mediated fibrinolysis
- Under the right circumstances (injury
etc.) endothelial cells produce inhibitors
of plasminogen activator (PAI's)
- Loss of endothelium reveals ECM
collagen-bound vWF -> platelets biond
vWF (via the platelet glycoprotein GPIb)
- Normally the endothelium prevents thrombus
formation by actively exhibiting antiplatlet,
anticoagulant and profibrinolytic properties
- Platelets
- Disc-shaped, anucleate cell
fragments (from megakaryocytes -
about 2-3,000 per megakaryocyte)
- Function depends on their activation;
shape change and degranulation
- Function depends on their activation;
shape change and degranulation
- Feature granules (alpha and delta granules)
- Alpha-granules feature P-selectins in
the membrane (become externalised
- adhesion); TGF-beta; PDGF;
fibronectin and coagulation factors
- Clotting factors in alpha-granules
= fibrinogen (I); V and VIII
- Clotting factors in alpha-granules
= fibrinogen (I); V and VIII
- Delta-granules contain ADP, ATP, ionised
Ca(2+), histamine, seratonin and adrenaline
- Alpha-granules feature P-selectins in
the membrane (become externalised
- adhesion); TGF-beta; PDGF;
fibronectin and coagulation factors
- Normally platelets
are inactivated
- Following vessel endothelial damage
- ECM (with vWF is exposed)
- Platelets bind to this via their
surface GPIb glycoprotein
- Also able to bind other ECM
components (e.g. fibronectin)
- Secretion of both alpha
and delta-granules
- Alpha-granule products
promote coagulation and
adhesion of platelets
- Delta-granule products
activate the coagulation
cascade (Ca(+) and ADP also
promotes platelet aggregation)
- Platelet aggregation at the injury site (aided
by ADP and thromboxane A2 (TxA2) release
- This aggregation leads to the formation
of the primary haemostatic plug
- Held together by the interaction
between platelets (GPIIb-IIIa -
fibrinogen - GPIIb-IIIa) and platelets
with the ECM (via ECM vWF - GPIb)
- This is followed by the activation of the
coagulation cacade which ultimately
produces fibrin (forms a meshwork
around the platelet aggregation)
- Platelets release coagulation factors (fibrinogen (I), V and VIII)
- Platelets release pro-coagulative factors (Ca(+))
- Platelets release coagulation factors (fibrinogen (I), V and VIII)
- Activated platelets contract
their cytoskeletons to form a
tight-knit mass of cells
- Held together by the interaction
between platelets (GPIIb-IIIa -
fibrinogen - GPIIb-IIIa) and platelets
with the ECM (via ECM vWF - GPIb)
- ADP activates other platelets
- Causes conformational change in a large
platelet surface glycoprtein (GPIIb-IIIa)
- GPIIb-IIIa binds fibrinogen
(from alpha-granules) and links
activated platelets together
- Loss = Glanzmann's
thrombasthenia (another
bleeding disorder)
- GPIIb-IIIa binds fibrinogen
(from alpha-granules) and links
activated platelets together
- Causes conformational change in a large
platelet surface glycoprtein (GPIIb-IIIa)
- TxA2 is a potent
vasoconstrictor
- This aggregation leads to the formation
of the primary haemostatic plug
- Alpha-granule products
promote coagulation and
adhesion of platelets
- Also able to bind other ECM
components (e.g. fibronectin)
- Loss of this factor results in von
willebrand disease (bleeding disorder)
- Loss of the GPIb receptor = Bernard-soulier
syndrome (bleeding disorder)
- Loss of the GPIb receptor = Bernard-soulier
syndrome (bleeding disorder)
- Platelets bind to this via their
surface GPIb glycoprotein
- ECM (with vWF is exposed)
- Following vessel endothelial damage
- Disc-shaped, anucleate cell
fragments (from megakaryocytes -
about 2-3,000 per megakaryocyte)
- Endothelium
- Testing
platelets
- Full blood count (with mean
platelet volume (MPV), blood film)
- PFA-100 (platelet
function analyser)
- Full blood sample is drawn up
through a capillary tube towards a
membrane with a hole in the end
- The membrane is coated in collagen
with either; ADP or adrenaline
- If normal platelets -> should be activated
by the membrane and form a clot
- Blood should be inhibited from
passing through the hole at the end
- Blood should be inhibited from
passing through the hole at the end
- If normal platelets -> should be activated
by the membrane and form a clot
- The membrane is coated in collagen
with either; ADP or adrenaline
- Measures high shear haemostasis
- Full blood sample is drawn up
through a capillary tube towards a
membrane with a hole in the end
- Platelet
aggregation
assay
- In vitro assays
- Measure platelets clumps in platelet-rich
plasma (PRP) or whole blood when
exposed to aggregation agonists
- Collagen, ADP and thrombin
all bind to their own specific
receptor resulting in activation
- All receptors are implicated in different
diseases (e.g. GPIb, GPIIb-IIIa)
- Activation = shape change,
granule release and aggregation
- All receptors are implicated in different
diseases (e.g. GPIb, GPIIb-IIIa)
- Collagen, ADP and thrombin
all bind to their own specific
receptor resulting in activation
- Measure platelets clumps in platelet-rich
plasma (PRP) or whole blood when
exposed to aggregation agonists
- Activation-induced
change depends on the
normal platelet function
- Useful data; lag phase,
aggregation rate and
amplitude
- Useful data; lag phase,
aggregation rate and
amplitude
- In vitro assays
- Platelet
secretion
assay
- Platelet ADP/ATP release (from
delta-granules) can be measured
- Valuable diagnostic tool
- Methods: HPLC (high performance
liquid chromatography) luminescence;
Firefly lantern preps (luminescence
due to the ATP concentration)
- Valuable diagnostic tool
- Platelet ADP/ATP release (from
delta-granules) can be measured
- Flow
cytometry
- Uses whole blood (2ul minimum) -
therefore its a physiological activity assay
- Whole blood sample prevents
artificially induced platelet aggregation
- Whole blood sample prevents
artificially induced platelet aggregation
- All blood cell properties can be analysed simultaneously
- (Not just platelets)
- (Not just platelets)
- New Ab's or dyes can be easily introduced into samples
- High degree of sensitivity
- Future - aggregation by flow?
- I have no idea what this means either...
- I have no idea what this means either...
- Future - aggregation by flow?
- Uses whole blood (2ul minimum) -
therefore its a physiological activity assay
- Full blood count (with mean
platelet volume (MPV), blood film)
- Examples
of platelet
disorders
- Thrombocytopaenia
- Signs/symptoms
- Common
- Spontaneous skin pupura (/ecchymoses)
- Mucous membrane bleeding (/epistaxis)
- Protracted bleeding after trauma/surgery
- Menorrhagia / postpartum haemorrhage
- Spontaneous skin pupura (/ecchymoses)
- Uncommon
- Haemorrhages in the following places
- Intracranial, gastrointestinal,
retinal and genitourinary
- Intracranial, gastrointestinal,
retinal and genitourinary
- Haemorrhages in the following places
- Common
- Causes
(aetiology)
- Drugs
- Infection
- DIC
- Immune
- Drugs
- Signs/symptoms
- Glanzmann's thrombasthenia
- Loss of platelet GPIIb-IIIa
(binds platelets together
via fibrinogen bridge)
- >40 mutations ID'd (most type I involve
the GPIIb gene; others = GPIIIa gene)
- >40 mutations ID'd (most type I involve
the GPIIb gene; others = GPIIIa gene)
- Bleeding disorder with a
normal platelet count
- Test results
- Normal
- Platelet count
- Platelet size / morphology
and lifespan
- Platelet count
- Very long bleeding
time and PFA result
- Normal
- Autosomal recessive
- Often severe bleeding,
but variable phenotype
- Subtypes (1 = complete IIb-IIIa
loss; 2 = partial loss of IIb-IIIa)
- Subtypes (1 = complete IIb-IIIa
loss; 2 = partial loss of IIb-IIIa)
- Often severe bleeding,
but variable phenotype
- Loss of platelet GPIIb-IIIa
(binds platelets together
via fibrinogen bridge)
- Treatment options in
platelet disorders
- Specialist care
- Avois aspirin, NSAIDs
- Hormonal control on menses
- Supportive care - tranexamic acid
- Platelet transfusion
- Recombinant rVIIIa
(clotting factor)
- Specialist care
- Thrombocytosis (=
high concentration of
platelets in the blood)
- Causes
- Inflammatory
response
- Fe-deficiency / bleeding
- Bone marrow
disorder (e.g. cancer)
- Inflammatory
response
- Antiplatelet /
anticoagulant
agents
- Heparin (binds antithrombin(III)
and inactivates thrombin)
- Aspirin, NSAIDs (inhibit COX2)
- Clopidogrel (ADP
receptor inhibitor)
- Heparin (binds antithrombin(III)
and inactivates thrombin)
- Causes
- Thrombocytopaenia
- Von willebrand factor (vWF)
- Large multimeric glycoprotein
(exists as a series of multimers)
- Extensively processed
(multimer assembly)
- Constituitively expressed
- Constituitively expressed
- Extensively processed
(multimer assembly)
- Functions
- Carrier protein for
factor VIII (protects VIII
against premature
proteolytic degradation)
- Adhesive protein in primary
haemostasis (platelet adhesion)
- Binds a number of ligands
- Collagen; platelet GPIb and
GPIIb-IIIa; sulfatides; heparin
- Collagen; platelet GPIb and
GPIIb-IIIa; sulfatides; heparin
- Carrier protein for
factor VIII (protects VIII
against premature
proteolytic degradation)
- Clinical
features
- Highly heterogenous
phenotypic expression
- Mild-moderate
bleeding tenedency
- Bruising, epistaxis,
gingival haemorrhage,
post-surgical/dental
bleeding
- Bruising, epistaxis,
gingival haemorrhage,
post-surgical/dental
bleeding
- Mucosal
bleeding
- Mild-moderate
bleeding tenedency
- Highly heterogenous
phenotypic expression
- Laboratory
diagnosis
- Screening test
- Increased bleeding time, increased
partial thromboplastin time (doesnt
invovle tissue factor)
- Increased bleeding time, increased
partial thromboplastin time (doesnt
invovle tissue factor)
- Specific assay
- Decreased: factor VIII, vWF
(via Ab) and vWF activity
- Decreased: factor VIII, vWF
(via Ab) and vWF activity
- Screening test
- Criteria
- Type 1 vWD
(von willebrand
disease)
- Inherited bleeding disorder
- Diagnosis based on three criterias -
symptoms, lab tests and inheritence pattern
- If all three criteria not met = possible type 1 VWD
- If all three criteria not met = possible type 1 VWD
- Diagnosis based on three criterias -
symptoms, lab tests and inheritence pattern
- Inherited bleeding disorder
- Type 1 vWD
(von willebrand
disease)
- Large multimeric glycoprotein
(exists as a series of multimers)
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