Download coagulation

Survey
yes no Was this document useful for you?
   Thank you for your participation!

* Your assessment is very important for improving the workof artificial intelligence, which forms the content of this project

page
1
page
2
page
3
page
4
page
5
page
6
page
7
page
8
page
9
page
10
page
11
page
12
page
13
page
14
page
15
page
16
page
17
page
18
page
19
page
20
page
21
page
22
page
23
page
24
page
25
page
26
page
27
page
28
page
29
page
30
page
31
page
32
page
33
page
34
page
35
page
36
page
37
page
38
page
39
page
40
page
41
page
42
page
43
page
44
page
45
Document related concepts

Gene therapy of the human retina wikipedia , lookup

Multiple sclerosis research wikipedia , lookup

Transcript 
Disseminated Intravascular Coagulation
DIC
Doç.Dr. Tiraje Celkan
DIC DEATH is COMING
• An acquired syndrome
characterized by
systemic intravascular
coagulation
• Coagulation is always the
initial event.
• Most morbidity and
mortality depends on
extent of intravascular
thrombosis
• Multiple causes
6
Thrombosis
Platelet
Red Blood Cell
Fibrin
WWW. Coumadin.com
DIC
Diseases……DIC
2 mechanism
•
•
•
•
Cytokines ….activated….coagulation activation
(sepsis and major traumas
Procoagulants ….. ın the blood stream
(malignancy and obstetric cases)
DIC
DIC pathogenesis
UYARAN
Monosit ve Makrofajlar
TF Salınımı
Sitokinler
Endotel
TF+ FVIIa
TFPI
Tenaz
Trombomodulin
Aktive Protein C
Protein S
ATIII
Protrombinaz
Trombomodulin
ATIII
HCII
Trombin
Endotelyel
prostasiklin
Trombosit agregasyonu
t-PA
Plazmin
Fibrin monomerleri
Hemostasis
•
•
•
•
Vascular Endothelium
Blood Flow Dynamics
Platelets
Coagulation cascade
• Anticlotting Mechanisms
• Fibrinolytic System
WWW. Coumadin.com
DIC
• An acquired
syndrome
characterized by
systemic
intravascular
coagulation
• Coagulation is always
the initial event
SYSTEMIC
ACTIVATION OF
COAGULATION
Intravascula
r deposition
of fibrin
Depletion of
platelets and
coagulation
factors
Thrombosis in
small and
midsize vessels
Bleeding
Organ failure
DEATH
Thrombotic
Probblems
Disease
Bleeding
Activation of coagulation
Fibrin in the
blood stream
Plt and factor
decrease
Thrombus in capillers
inhibition of
fibrinolizis
Fibrin
Organ
Failure
activation of
fibrinolizis
FDP formation
Bleeding
DF + FVIIa
FIXa + (FVIII)
• AT-III level decrease
• Sürekli trombin oluşumuna bağlı tüketim
• Aktive nötrofillerden salınan elastaza bağlı yıkım
• AT sentezinin bozulması
• Protein C
•
Endotelde trombomodulin sunumunda azalma
• PC sentezinde bozulma
• Serbest PS düzeyinde azalma
• TFPI decrease
• TFPI düzeyi normal
FXa + (FV)
Thrombin
Fibrinogen
Fibrin
trombin formation
(DF)
Decreased
anticoagulatıon
Fibrin formation
Thrombus in capillers
DF + FVIIa
PAI-1
FIXa + (FVIII)
FXa + (FV)
Plazminojen
Plazminojen
aktivatörleri
Trombin
Fibrinojen
trombin oluşumu
(DF aracılığı ile)
Fibrin
Plazmin
AT-III düzeyinde düşüklük
Protein C sisteminde bozulma
TFPI yetersizliği
Antikoagülan sistemde
yetersizlik
Fibrin oluşumu
Fibrin
Fibrinolitik sistemin
baskılanması (PAI-1 ile)
Fibrin uzaklaştırılmasında
yetersizlik
Küçük ve orta çaplı
damarlarda trombüs
FYÜ
Hemostatic Balance
PAI-1
Antiplasmin
Tissue factor*
Prot. S
Prot. C
TFPI
Fibrinolytic System
Clotting Factors
Procoagulant
ATIII
Anticoagulant
Pathophysiology of DIC
• Activation of Blood Coagulation
• Suppression of Physiologic
Anticoagulant Pathways
• Impaired Fibrinolysis
• Cytokines
Pathophysiology of DIC
• Activation of Blood Coagulation
– Tissue factor/factor VIIa mediated
thrombin generation via the extrinsic
pathway
• complex activates factor IX and X
– TF
• endothelial cells
• monocytes
• Extravascular:
– lung
– kidney
– epithelial cells
Pathophysiology of DIC
• Suppression of Physiologic
Anticoagulant Pathways
– reduced antithrombin III levels
– reduced activity of the protein C-protein S
system
– Insufficient regulation of tissue factor
activity by tissue factor pathway inhibitor
(TFPI)
• inhibits TF/FVIIa/Fxa complex activity
Pathophysiology of DIC
• Impaired Fibrinolysis
– relatively suppressed at time of maximal
activation of coagulation due to increased
plasminogen activator inhibitor type 1
Pathophysiology of DIC Cytokines
• Cytokines
– IL-6, and IL-1 mediates coagulation activation in DIC
– TNF-
• mediates dysregulation of physiologic anticoagulant
pathways and fibrinolysis
• modulates IL-6 activity
– IL-10 may modulate the activation of coagulation
Inflamation
Coagulation
Diagnosis of DIC
Presence of disease associated with
DIC
Appropriate clinical setting
– Clinical evidence of thrombosis,
hemorrhage or both.
Laboratory studies
– no single test is accurate
– serial test are more helpful than single test
Conditions Associated With
DIC
• Malignancy
– Leukemia
– Metastatic disease
• Cardiovascular
– Post cardiac arrest
– Acute MI
– Prosthetic devices
• Hypothermia/Hyperth
ermia
• Pulmonary
– ARDS/RDS
– Pulmonary
embolism
• Severe acidosis
• Severe anoxia
• Collagen vascular
disease
• Anaphylaxis
Conditions Associated With
DIC
• Infectious/Septicem
ia
– Bacterial
• Gm - / Gm +
– Viral
• CMV
• Varicella
• Hepatitis
– Fungal
• Intravascular
hemolysis
• Acute Liver Disease
• Tissue Injury
–
–
–
–
trauma
extensive surgery
tissue necrosis
head trauma
• Obstetric
–
–
–
–
Amniotic fluid emboli
Placental abruption
Eclampsia
Missed abortion
Clinical Manifestations of DIC
ORGAN
Skin
Ischemic Findings
are earliest!
CNS
Renal
Cardiovascular
Pulmonary
GI
Endocrine
ISCHEMIC
HEMOR.
Pur. Fulminans
Gangrene
Acral cyanosis
Delirium/Coma
Infarcts
Oliguria/Azotemia
Cortical Necrosis
Myocardial
Dysfxn
Dyspnea/Hypoxia
Infarct
Ulcers, Infarcts
Adrenal infarcts
Petechiae
Echymosis
Oozing
Intracranial
bleeding
Hematuria
Hemorrhagic
lung
Massive
hemorrhage.
Bleeding is the most
obvious
clinical finding
Clinical Manifestations of DIC
Microscopic findings in DIC
• Fragments
• Schistocytes
• Paucity of platelets
Laboratory Tests Used in DIC
•
•
•
•
•
•
D-dimer*
Antithrombin III*
F. 1+2*
Fibrinopeptide A*
Platelet factor 4*
Fibrin Degradation
Prod
• Platelet count
• Protamine test
•
•
•
•
•
•
•
Thrombin time
Fibrinogen
Prothrombin time
Activated PTT
Protamine test
Reptilase time
Coagulation factor
levels
*Most reliable test
Laboratory diagnosis
• Thrombocytopenia
– plat count <100,000 or rapidly declining
• Prolonged clotting times (PT, APTT)
• Presence of Fibrin degradation
products or positive D-dimer
• Low levels of coagulation inhibitors
– AT III, protein C
• Low levels of coagulation factors
– Factors V,VIII,X,XIII
• Fibrinogen levels not useful
Differential Diagnosis
•
•
•
•
•
•
Severe liver failure
Vitamin K deficiency
Liver disease
Thrombotic thrombocytopenic purpura
Congenital abnormalities of fibrinogen
HELLP syndrome
Treatment of DIC
• Stop the triggering process .
– The only proven treatment!
• Supportive therapy
• No specific treatments
– Plasma and platelet substitution therapy
– Anticoagulants
– Physiologic coagulation inhibitors
Plasma therapy
• Indications
– Active bleeding
– Patient requiring invasive procedures
– Patient at high risk for bleeding complications
• Prophylactic therapy has no proven
benefit.
• Cons:
• Fresh frozen plasma(FFP):
– provides clotting factors, fibrinogen, inhibitors,
and platelets in balanced amounts.
– Usual dose is 10-15 ml/kg
Platelet therapy
• Indications
– Active bleeding
– Patient requiring invasive procedures
– Patient at high risk for bleeding complications
• Platelets
– approximate dose 1 unit/10kg
Blood
• Replaced as needed to maintain
adequate oxygen delivery.
– Blood loss due to bleeding
– RBC destruction (hemolysis)
Coagulation Inhibitor Therapy
•
•
•
•
Antithrombin III
Protein C concentrate
Tissue Factor Pathway Inhibitor (TFPI)
Heparin
Antithrombin III
• The major inhibitor of the coagulation
cascade
– Levels are decreased in DIC.
– Anticoagulant and antiinflammatory properties
• Therapeutic goal is to achieve supranormal
levels of ATIII (>125-150%).
– Experimental data indicated a beneficial effect
in preventing or attenuating DIC in septic shock
• reduced DIC scores, DIC duration, and some
improvement in organ function
– Clinical trials have shown laboratory evidence of
attenuation of DIC and trends toward improved
Protein C Concentrates
• Inhibits Factor Va, VIIa and PAI-1 in
conjunction with thrombomodulin.
• Protein S is a cofactor
• Therapeutic use in DIC is experimental and is
based on studies that show:
– Patients with congenital deficiency are prone to
thromboembolic disease.
– Protein C levels are low in DIC due to sepsis.
– Levels correlate with outcome.
– Clinical trials show significantly decreased
morbidity and mortality in DIC due to sepsis.
Tissue Factor Pathway
Inhibitor
• Tissue factor is expressed on endothelial
cells and macrophages
• TFPI complexes with TF, Factor VIIa,and
Factor Xa to inhibit generation of thrombin
from prothrombin
• TF inhibition may also have antiinflammatory
effects
• Clinical studies using recombinant TFPI are
promising.
Heparin
• Use is very controversial. Data is mixed.
• May be indicated in patients with
clinical evidence of fibrin deposition or
significant thrombosis.
• Generally contraindicated in patients
with significant bleeding and CNS
insults.
• Dosing and route of administration
varies.
• Requires normal levels of ATIII.
Antifibrinolytic Therapy
• Rarely indicated in DIC
– Fibrinolysis is needed to clear thrombi from the
micro circulation.
– Use can lead to fatal disseminated thrombosis.
• May be indicated for life threatening bleeding
under the following conditions:
– bleeding has not responded to other therapies and:
– laboratory evidence of overwhelming fibrinolysis.
– evidence that the intravascular coagulation has
ceased.
• Agents: tranexamic acid, EACA
Summary
• DIC is a syndrome characterized systemic
intravascular coagulation.
• Coagulation is the initial event and the extent of
intravascular thrombosis has the greatest impact on
morbidity and mortality.
• Important link between inflammation and coagulation.
• Morbidity and mortality remain high.
• The only proven treatment is reversal or control of
the underlying cause.
In Normal conditions
• Thrombin....endotelium....TM....TM+
thrombin ....Pr. C act....act FV and
FVIII inact
• TM+ thrombin.......fibrin formation
decresed
Sepsis
Coagulation activation
Anticoagulation act. decrease
Inhibition of Fibrinolizis
IL-6
TNF
sepsis
•
•
•
•
Plazminogen decreased
fibrin deposition in tissues
fibrinolitic act. İnsufficient
multi system involvement
Sepsis
•
•
•
•
•
Endotelium …. TM decreased
TM dec……… Pr C activation decreased
Pr C decreased in blood
Fibrinolizis decreased
Thrombus increased (APC FV, FVIII
protrombinaz and tenaz inhibition)
Clinics
• Bleeding
70-90 % of patients
skin (petechia, echimozis , hematomas)
GIS
GUS (hematuria, vaginal)
Pulmoner
catheter and from surgery lesions
• Thromboembolic complications
10-40 % of patients
especially in cancer patients
tissue and organ disfunction
Laboratory 1
• Screening tests
platelet count
Protrombin time
aPTT
Trombin time
Fibrinogen level
easy , cheap could be done every where
Laboratory 2
• Tests to evaluate Thrombin formation
D-dimer
Fibrin Monomers
Fibrinopeptide A
Prothrombin fragment 1-2
Trombin-Antitrombin
complicated
could not be done in every lab
more spesific for diagnosis
New tx
•
•
•
•
•
rTFPI ( Tifacogin )
APC ( Drotecogin )
Recombinant TM
AT3 ( Atenativ and Kybernin)
C1 inhibitor : C1 PK, and FXII inhibitor
Summary
•
•
•
•
•
DIC systemic intravaskular coagulation
coagulation …..vascular thrombosis
Enflamation….. coagulation
Morbidity and mortality
The best treatment to treat the basic reason
Related documents
Thrombosis and Hemostasis Societies of North America April 15
Thrombosis and Hemostasis Societies of North America April 15
Detecting Blood Coagulation On-Chip USF Available Technologies
Detecting Blood Coagulation On-Chip USF Available Technologies
Cardiovascular 19 – Homeostasis and Thrombosis
Cardiovascular 19 – Homeostasis and Thrombosis
i: leukocytes, volume, erythrocytes, suspended
i: leukocytes, volume, erythrocytes, suspended
Document
Document
No Slide Title - University of Windsor
No Slide Title - University of Windsor
Suppl. Table
Suppl. Table
Document
Document
The Modern Coagulation Cascade and Coagulation
The Modern Coagulation Cascade and Coagulation
CESO_SEMINARS_2002_AMT_Presentation_June_10_02
CESO_SEMINARS_2002_AMT_Presentation_June_10_02