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COAGULATION

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The body's intrinsic ability to slow down or stop hemorrhage ... PF-3 serves as a binding site for cofactor V & VIII. production of thrombin. C. O. L. L ... – PowerPoint PPT presentation

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Title: COAGULATION

1
COAGULATION

Masatoshi Kida, M.D.
Dept. of Pathology
University of Vermont

2
HEMOSTASIS

The bodys intrinsic ability to slow down or stop
hemorrhage
normal hemostasis involves a delicate balance
between factors that promote blood coagulation
and thrombus stabilization and factors that
inhibit blood coagulation and promote thrombus
dissolution

RESOLUTION
FORMATION
clot
3
COAGULATION

vascular wall
coagulation factors
platelet

4
COAGULATION
FIRST STEP

Smooth muscle
muscle constriction
luminal diameter reduction
retarding blood loss
enhancing platelet adherence
Endothelial cells
VIII-vWF synthesis
thromboplastin (III) release
? activation of ext pathway
activation of Factor IX X
Subendothelium
collagen ? platelet adherence, activation

5
PRIMARY HEMOSTASIS

Platelet
Adherence
Activation
Aggregation
(Contraction)
(Stabilization)

6
Platelet Adhesion
mediated by GP-Ib on platelet surface and vWF
fibrinogen
C O L L A G E N
C O L L A G E N
GP-Ib
von Willebrand Factor
endothelial cells
7
von Willebrand Factor

Synthesized stored in endothelial cells and
megakaryocytes (also stored in platelets)
Forming bridge between subendothelial collagen
and Plt
Carrier molecule for Factor VIII Coagulant
Protein (vWF is also known as Factor VIII
Related Antigen)
Circulates as series of multimers (in various
sizes)
Large, high molecular weight multimers required
for normal hemostasis

8
Platelet Activation
release of a and electron dense granules

Release of platelets cytoplasmic products
activation of platelet factor III (PF-3)
PF-3 serves as a binding site for cofactor V
VIII
production of thrombin

C O L L A G E N
GP-IIb, IIIa
9
Platelet Aggregation
GP IIb-IIIa - fibrinogen interaction

formation of primary plug
activated platelets synthesize and secrete TXA2
TXA2
1. promotes plt aggregation
2. vasoconstriction
3. release of plt factor (ADP)

C O L L A G E N
Aspirin inhibits TXA2 and ADP
10
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11
Coagulation Factors
XII
XI
IX
extrinsic pathway
intrinsic pathway
VIII
VII
X
V
PT
aPTT
I
XIII
Stable clot
12
Coagulation Factors
negative charged surface
XII

Intrinsic Pathway
Extrinsic Pathway
Common Pathway
majorities are serine proteases
circulate as inactive forms (require activation
to function)
majority produced in liver

XI
tissue factor
IX
intrinsic pathway
extrinsic pathway
VIII
VII
X
V
PT
aPTT
II
I
XIII
Stable clot
13
Coagulation Factors
negative charged surface

Intrinsic Pathway
Extrinsic Pathway
Common Pathway
majorities are serine proteases
circulate as inactive forms (require activation
to function)
majority produced in liver
many require vit K for synthesis
II, VII, IX, X
protein C, S

XII
XI
tissue factor
IX
intrinsic pathway
extrinsic pathway
VIII
VII
X
V
PT
aPTT
II
I
XIII
Stable clot
14
Secondary Hemostasis

tissue factor
phospholipid complex
thrombin activation
fibrin polymerization
thrombin, ADP, TXA2
Contraction
contraction of intraplatelet actomyosin
formation of secondary plug
uncover plt membrane receptors (GPIb, IIIa)
Stabilization
activation of XII thrombin
cross linking of fibrin monomers

15
A
A
fibrinopeptide A B
fibrinogen
B
B
D domain
E domain
fibrin monomer
Spontaneous aggregation
soluble fibrin polymer
16
Stabilization of Fibrin Clot
soluble fibrin clot
Thrombin
Factor XII I Factor XIIIa
stabilized fibrin clot
17
Other Proteins in Blood Coagulation

Prekallikrein
activates XII and prekallikrein
High molecular wt. Kininogen (HMWK) (binding
protein)
supports reciprocal activation of XII, XI and
prekallikrein

18
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19
ANTICOAGULATION FIBRINOLYSIS

Vascular Wall
Anti-Coagulation Factors
Fibrinolytic Factors

20
ANTICOAGULATION FIBRINOLYSISVascular Wall

Endothelial Cell
prostacyclin (PGl2)
heparan sulfate
thrombomodulin
tissue plasminogen activator (tPA)
Muscle
muscular dilation

21
ANTICOAGULATION FIBRINOLYSISAnti-Coagulation
Factors

Antithrombin III (with thrombin heparin)
negative feedback on thrombin
inactivates Xa (XIIa, XIa, IXa)
Prostacyclin (PGl2) from endothelial cells
vasodilation
conversion of ADP into products that inhibit plt
aggregation
thrombin endothelial cells
thrombomodulin binds activates Protein C
inactivates Va VIIIa
inhibits thrombin

XII
XI
IX
VIII
VII
X
V
II
I
XIII
Stable clot
22

Protein C
vit K dependent zymogen
produced in liver
inactivates Va and VIIIa
Protein S
vit K dependent binding protein
co-factor for protein C
binds C4b-binding protein

XII
XI
IX
VIII
VII
X
V
II
I
XIII
Stable clot
23
AnticoagulationHeparin

Heparin activates Antithrombin III (AT III)
AT III inactivates Thrombin and Factor Xa
rapid onset of action
Laboratory monitoring
aPTT 1.5X 2.5X normal mean
heparin level
0.2 0.4 U/mL by protamine titration
0.35 0.70 by Factor Xa inactivation assay

XII
XI
IX
VIII
VII
X
aPTT
V
II
I
XIII
Stable clot
24
AnticoagulationHeparin
AT
AT
25
II
26
AT
II
27
II
AT
28
AT
II
29
AT
II
30
AT
II
31
Coumadin (Warfarin) Anticoagulants
XII

inhibits hepatic synthesis of vit K-dependent
clotting factors (II, VII, IX, X)
competitive inhibition of g-carboxylation
inactivate acarboxy forms synthesized
onset delayed 3 to 5 days
also inhibits synthesis of protein C S

XI
IX
VIII
VII
X
V
PT
II
I
XIII
Stable clot
32
Thrombolytic (Fibrinolytic) Factors

Urokinase released from endothelial cells and
monocytes
Tissue plasminogen activator (tPA)
conversion of plasminogen to plasmin
cleavage of fibrinogen fibrin into
fibrin split products
inhibit plt aggregation
thrombin activity
fibrin strands cross linking

33
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34
Plasmin Degradation of Fibrin Clot
plasmin
plasmin
plasmin
Fibrin Degradation Products
D-dimer
DED complex
E-fragment
35
Bleeding Disorders
36
Procoagulant Platelets Factors Fibrinogen von
Willebrand Factor
Profibrinolytic Plasminogen tPA Fibrin Fragment
D-dimer
RESOLUTION
FORMATION
clot
Anticoagulant Antithrombin III Protein C Protein S
Antifibrinolytic PAI-1 Alpha-2 Antiplasmin
37
Vessel Abnormalitiesincreased vascular fragility

manifested by petechial hemorrhages of
skin/mucous membranes
bleeding time, plt count, PT, aPTT --- normal
not life threatening bleeding
1. congenital
a. Ehlers-Danlos syndrome (AD)
b. hereditary hemorrhagic telangiectasia (AD)
2. acquired
a. hypersensitivity vasculitis
(1) drug reaction immune complex deposit in
vessel walls
(2) Henoch-Schonlein purpura
b. scurvy (vit C deficiency)

38
Henoch-Schonlein purpura

generalized hypersensitivity vasculitis
uncertain cause
clinical Sx
purpura
colicky abdominal pain
polyarthralgia
acute glomerulonephritis

39
Coagulation Factor Abnormality

hematomas/ecchymoses after minor trauma
often severe bleeding
1. congenital usually single factor deficiency
a. sex-linked
(1) hemophilia A (Factor VIII def.)
(2) hemophilia B (Christmas disease, Factor IX
def.)
b. autosomal dominant
(1) von Willebrands disease
c. autosomal recessive
2. acquired usually multi-factor deficiency and
clotting abnormalities
a. vitamin K deficiency
b. severe liver disease

40
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41
Hemophilia A (Factor VIII deficiency)

bleeding into joints ? crippling arthropathy
sex-linked inheritance
high rate of spontaneous mutation
25 of pts do not have family history of
hemophilia
decreased VIII-C, near normal VIII-vWF
gt50 severe deficiency
increased aPTT
normal bleeding time, plt, PT

XII
XI
IX
VIII
VII
X
aPTT
V
II
I
XIII
Stable clot
42
hemophilia A
43
Hemophilia B(Christmas disease, Factor IX def.)

less common than hemophilia A
similar clinical Sx and inheritance pattern as
hemophilia A (sex-linked)

XII
XI
IX
VIII
VII
X
V
II
I
XIII
Stable clot
44
von Willebrands disease

easy bruisability (no bleeding into joints)
unable to release VIII-vWF
intact VIII-vWF synthesis
VIII-C level is also decreased (unknown reason)
autosomal dominant
1 in 30,000 population
usually diagnosed in childhood or young adults
increased bleeding time
normal plt, PT
normal or increased aPTT

45
Vitamin K Deficiencyvitamin K dependent factors
II, VII, IX, X

acquired disorder
may occur in malnutrition, malabsorption, biliary
obstruction, drug
increased PT
normal bleeding time, plt
normal or increased aPTT

XII
XI
IX
VIII
VII
X
V
PT
II
I
XIII
Stable clot
46
Severe Liver Diseasefactors synthesized in
liver II, V, VII, IX, X, fibrinogen
XII

increased PT, aPTT
normal bleeding time, plt

XI
IX
VIII
VII
X
V
PT
aPTT
II
I
XIII
Stable clot
47
PLATELET ABNORMALITIES

1. Thrombocytopenia
a. decreased production
b. increased utilization
c. increased destruction
(1) isoimmune thrombocytopenia
(2) idiopathic thrombocytopenic purpura (ITP)
(3) thrombotic thrombocytopenic purpura (TTP)
(4) drug reaction
(5) mechanical destruction
(6) hypersplenism
2. Functional abnormalities
a. congenital
(1) defective adhesion (Bernard-Soulier)
(2) defective aggregation (thrombasthenia)
b. acquired
(1) aspirin
(2) thrombocythemia

48
Thrombocytopenia

decreased in number of platelets
bleeding from small vessels (skin, GI, mucous
membrane, GU, brain)
normal or increased bleeding time
decreased platelet
normal PT, aPTT

49
Thrombocytopenia

decreased production
diffuse bone marrow disease (aplastic anemia,
tumor)
megakaryocyte disorder
increased utilization
DIC

50
Thrombocytopenia
increased destruction

isoimmune thrombocytopenia
neonatal
PLA 1 neg. mother PLA 1 pos. baby
production of anti-PLA 1 Ab (IgG)
post-transfusion
PLA 1 neg. recipient PLA 1 pos. platelet
destruction of PLA 1 platelets and recipient's
own platelets

51
Thrombocytopenia
increased destruction

idiopathic thrombocytopenic purpura (ITP)
acute ITP
children following a viral infection
self-limiting disease
? platelet as an innocent bystander
chronic ITP
adults (often premenopausal females)
may be associated with other autoimmune
diseases
production of autoantibody against Pts own
platelets
removal of opsonized platelets by
reticuloendothelial system
decreased circulating platelet, but increased BM
megakaryocytes

idiopathic thrombocytopenic purpura (ITP)
clinical
easy bruising and bleeding after minor trauma
treatment
steroid
splenectomy

53
Thrombocytopenia
increased destruction

thrombotic thrombocytopenic purpura (TTP)
abnormal platelet aggregation in microcirculation
microangiopathic hemolytic anemia
fever
transient neurologic deficits
renal failure
hemolytic uremic syndrome (HUS)
platelets start to aggregate in small vessels
without particular reason

54
Disseminated Intravascular Coagulation (DIC)

- an acute, subacute, or chronic
thrombohemorrhagic disorder occurring as a
secondary complication in a variety of diseases
- activation of clotting system resulting in wide
spread formation of microthrombi throughout the
microcirculation
- as a consequence, causing consumption of
platelets, fibrin and coagulation factors, and
activation of thrombolytic mechanism
Two major triggering mechanisms
1. release of tissue factor or thromboplastic
substance
2. widespread endothelial injury

55
DIC

Triggering Mechanisms
1. release of tissue factor or thromboplastic
substance
- placental tissue
- granules from leukemic cells
- bacterial endotoxin
- mucus from adeno CA
2. widespread endothelial injury
- Ag-Ab immune complex deposit
- extreme temperature
- microorganisms

56
DIC

Pathology - wide spread thrombi
(brain, heart, lungs, kidneys, adrenals,
spleen , liver)
- microinfarcts
Clinical - 50 associated with obstetric
complications
- 30 with carcinomatosis
- microangiopathic anemia
- dyspnea, cyanosis
- convulsions, coma
- oliguria, acute renal failure
- shock, circulatory failure

57
DIC

Clinical acute DIC with a predominance of
thrombin generation and consumption of
coagulation factors
bleeding tendency
(oozing from venopuncutres or operating site)
subacute and chronic DIC
thrombotic tendency

58
DIC