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BLEEDING DISORDERS

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BLEEDING DISORDERS Dr.Nazzal Bsoul Hematologist Al Bashir Hospital Therapies other than replacement therapy Ice. Immobilization. Steroids. Physiotherapy. – PowerPoint PPT presentation

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Title: BLEEDING DISORDERS

1

BLEEDING DISORDERS
Dr.Nazzal Bsoul
Hematologist
Al Bashir Hospital

2
HEMOSTASIS-1

In health hemostasis ensures that the blood
remains fluid and contained in the vasc.system.
If a vessel wall is damaged,a number of
mechanisms are activated promptly to limit
bleeding,involving
1-Endothelial cells.
2-Platelets.
3-Plasma coag.factors.
4-Fibrinolytic system.

3
HEMOSTASIS-2

These activities are finely balanced between
keeping the blood fluid and preventing
intravasc.thrombosis.
1-Pimary hemostasis vasoconstriction and
platelet adhe-
sion and aggregation leading to the
formation of the
platelet plug.
2-Secondary hemostasis involves activation of
coag.sys-
tem leading to the generation of fibrin
strands and
reinforcement of the platelet plug.
3-Fibrinolysis activation of fibrin-bound
plasminogen resulting in clot lysis.

4
ROLE OF ENDOTHELIAL CELLS IN HEMOSTASIS

Blood vessels are lined with endothelial
cells,which synthesize and secrete various
agents,that regulate hemostasis.
1-Procoagulant(prothrombotic) agentstissue
factor,von Willebrand factor,F V ,F VIII.
2-Anticoagulant (antithrombotic) agents
prostacyclin,nitric oxide,endothelin-1.

5
ROLE OF PLATELETS IN HEMOSTASIS

Each megacaryocyte produces 1000-2000
platelets,which
remain in the circulation for about 10 days.
Releasing of hemostatic proteins.
Platelet adhesion.
Platelet aggregation.

6
COAGULATION FACTORS

Coag.factorsare plasma proteins synthesized in
the liver which,when activated lead to the
deposition of fibrin.
1-Initiation phaseleads to the formation of the
complex TF-VIIa.
2-Amplification phaseleads to the formation of a
small amount of thrombin from prothrombin.
3-Propagation phaseleads to the formation of
much larger amounts of fibrin.

7
INHIBITORS OF COAGULATION

Are proteins that inhibit activated
procaog.enzymes and prevent excessive
intravasc.coagulation
Raised levels are not associated with
bleeding.
Reduced levels may predispose to thrombosis.
Antithrombin.
Protein C,Protein S.
Tissue Factor Pathway Inhibitor (TFPI).

8
FIBRINOLYSIS

Small amouns of fibrin are constantly deposited
within the vascular system and are removed by the
fibrinolytic system
Plasminogen Plasmin
Fibrin
FDPs

9
ASSESSMENT OF BLEEDING SYMPTOMS

1-Careful and full clinical history and
examination.
2-Appropriate lab.investigations.
3-Other investigations.

10
HISTORY

1-Site of bleeding.
2-Duration of bleeding.
3-Precipitating cause.
4-Surgery.
5-Family history.
6-Systemic illnesses.
7-Drugs.

11
Clinical Features of Bleeding Disorders

Platelet Coagulation disorders factor
disorders
Site of bleeding Skin Deep in soft tissues
Mucous membranes (joints, muscles)
(epistaxis, gum,
vaginal, GI tract)
Petechiae Yes No
Ecchymoses (bruises) Small, superficial Large,
deep
Hemarthrosis / muscle bleeding Extremely
rare Common
Bleeding after cuts scratches Yes No
Bleeding after surgery or trauma Immediate, Delaye
d (1-2 days),
usually mild often severe

12
Coagulation factor disorders

Inherited bleeding disorders
Hemophilia A and B
vonWillebrand disease
Other factor deficiencies

Acquired bleeding disorders
Liver disease
Vitamin K deficiency/warfarin overdose
DIC

HEMOPHILIAS

14
Definition

Hemophilias are a group of related bleeding
disorders that most commonly are
inherited.
When the term hemophilia is used, it most
often refers to the following two
disorders
1- Factor VIII deficiency hemophilia A
2- Factor IX deficiency hemophilia B
(Christmas
disease)
Factor XI deficiency hemophilia C.

15
History

Hemophilia has featured prominently in
European royalty and thus sometimes
known as the royal disease.
Queen Victoria passed the mutation for
hemophilia B to her son Leopold, and
through some of her daughters, to
various royals across the continent,
including the royal families of Spain,
Germany, and Russia.

16
Clinical Manifestation

They exhibit a range of clinical severity
that correlates well with factor levels.
Severe disease factor activity less than
1
Moderate disease factor activity 1-5
Mild disease factor activity more than 5

17
Incidence and Inheritance-1

The combined incidence of hemophilia A
and B is 1 in 5000 live male births.
Approximately 80 have hemophilia A,2/3
of whom have severe disease.
Hemophilia A is the second most common
inherited bleeding disorder.
Severe cases among patients with hemophilia
B are less common (about ½)
Hemophilia A and B are X-linked recessive
diseases.

18
Incidence and inheritance-2
Slide 18
Slide 18

Factor VIII and IX are localized on X
Chromosome
Haemophilia A and B are caused by a defect on
the X chromosome
Affect almost exclusively men
Affect equally all races and ethnic groups

Male
Female
Carrier female
Male with Haemophilia
19
X-Linked Recessive Inheritance
Father With Haemophilia Father With Haemophilia Father With Haemophilia
X Y
X XX XY
X XX XY
Healthy Father Healthy Father Healthy Father
X Y
X XX XY
X XX XY
Healthy Mother
Carrier Mother
50 of daughters will be carriers 50 of sons
will have hemophilia
All daughters will be carriers All sons will
be healthy
20
Initial presentation-1

The majority of patients are known to have
hemophilia because of the family
history.
The majority of newborns with severe
hemophilia traverse delivery and the
first few months of life without
detection.
Early bleeding occurs commonly in association
with circumcision.

21
Initial presentation-2

The majority of newborns with severe
hemophilia become symptomatic during
the first 2 years of life.
Mean age at diagnosis of severe hemophilia
9 months,moderate disease 22 months.
Moderate and mild hemophilia may,in the
absence of informative family history,go
undetected for signficant periods of time
(age
14-62 years).

22
Sites of bleeding

As children begin to ambulate,bleeding episodes
occur more often and begin to involve
joints
and muscles,as well as other systems
1-Hemarthrosis is a painful,debilitatin
g
manifestation of hemophilia.
2-Skeletal musclehematoma formation
most
affects quadriceps,iliopsoas,and
forearm.
3-CNSintracranial hemorrhage.

23
Hemarthrosis (acute)
24
Diagnosis

Family history mainly on the maternal
side of the family.
Screening tests.
Specific factor assay, genetic testing.

25
Family history

The patients mother is a known carrier.
Negative family history in about 1/3 of patients.
Lack of a family history is of little value in
excluding the possibility of hemophilia.
1-spontaneous mutation which occurs
25-33 of cases.
2-Neonatal deaths or a passage of the
trait through a succession of female
carriers

26
Screening tests

Initial tests to be done in patients with a
bleeding diathesis of unknown etiology
1-Platelet count
2-Prothrombin time (PT).
3-Activated partial thromboplastin time
(aPTT).
A normal platelet count,normal PT,and a
prolonged aPTT is characteristic of
hemophilias, and heparin therapy.

27
Specific assays

Factors that can produce an isolated
prolonged aPTT are F VIII,F IX,and FXI
Genetic analysis of F VIII and F IX.
Prof.Abbadi did genetic studies to the all
Jordanian patients with hemophilia and
identified new novel mutations among
Jordanians with hemophilia A and B.

28
Hemophilia in females

Symptomatic hemophilia has been well-
documented in females.
Three possible explanations for this
1-X-chromosome inactivation in early
stage of embryogenesis.
2-Mating between an affected male and
a carrier female produces homozygous
disease in ½ of female offspring.
3-Abnormal karyotype (Turner syndrome)

29
Late complications

1-Joint destruction due to hemarthroses,
leading to a number of orthopedic
abnormalities (hemophilic osteo-
arthropathy).
2-Transmission of blood-borne infections.
3-Development of inhibitor antibodies.

30
Hemophilic arthropathy

Multiple factors may contribute to synovitis and
joint destruction in patints with
hemarthroses.
1- Tissue deposition of iron
2- Dense fibrosis of the joint with
contractures,pain,and limitation
of
motion.
Primary prophylactic treatment with factor
concentrates can markedly reduce the risk
of subsequent arthropathy.
Synovectomy pharmacological synovectomy.
radioactive
synovectomy.

31
Infection

Patients treated with older factor VIII and IX
concentrates were at high risk for
infection
with hepatitis A,B,C,and D and with
HIV.
The risk of infection has been reduced markedly
by improvement in donor screening and
virucidal techneques and the
development
of recombinant products.

32
Inhibitors

Antibodies are primarily IgG.
Occur in 25 of severe hemophilia A,and
3-5 of those with severe hemophilia B.
Much less common in patients with mild or
moderate disease.
Increased risk of bleeding.
Maturational delays.

33
Management-1

Complex, and should include
1-Preventive and comprehensive care.
(routine immunizations,circumcision,
dental care,counselling and
education,exercise and athletic
participation)
2-Replacement therapy (treatment
and prophylaxis)
3-Other therapies gene therapy.

34
Therapies other than replacement therapy

Ice.
Immobilization.
Steroids.
Physiotherapy.
Analgesia aspirin and NSAIDs are
contraindicated, paracetamol or codeine can be
used.
Desmopressin.
Antifibrinolytic therapy tranexamic
acid,epsilon
aminocaproic acid.

35
Treatment of hemophilia A