New Trends In The Management Of Bleeding Disorders - PowerPoint PPT Presentation

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New Trends In The Management Of Bleeding Disorders

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Title: New Trends In The Management Of Bleeding Disorders

1
New Trends In The Management Of Bleeding Disorders

Galila Zaher
MRCPath
Consultant Hematologist
KAUH

2
Congenital Bleeding disorders

VWD
Hemophilia A
Hemophilia B
Other congenital factor deficiency
Bernard Solier syndrome
GlanzmanThrombathenia
Storage pool defect

3
Acquired Bleeding Disorders

Coagulation Factor
Liver Disease
DIC
Consumptions Coagulopathies
Vitamin K deficiency
Platelets defects
ITP
Renal impairment
Myelo-proliferate Disorders

4
Hemophilia

A F VIII deficiency
B F IX deficiency
Affects one in 6000 males
A is 5 X gt B
Mild gt5,Moderate 2 -5, severe lt 2
Levels remain stable throughout life
Both HA HB are X linked

5
Clinical presentation

lt 2 years joint bleeds
Rare
Only bruising or mouth bleeds are seen
Head injuries are a major concern
gt 2 years
Joint and muscle bleeds become more common

6
Indication For Replacement

All joint bleeds Pain, swelling ,warmth or loss
of movement .
Muscle bleeds severe pain or are in a dangerous
location
Bruises usually dont need treatment

7
Treatment

Keep weight off of joint
Ice pack
Factor replacement - the sooner the better
Amicar or tranexamic acid mouth bleed

8
Factor replacement

Derived from pooled human plasma
Derived from pig (porcine) plasma
Recombinant products

9
Factor VIII (AHF)

Mechanism of action
No tool to predict the efficacy
Allergic reactions
Transient (short t ½)
Expensive.
Risk of transmission of infection

10
Biotech Development of Recombinant Factors
Amplification
Human FVII gene
hF Gene
Single copyof gene isolated
Liver gene library
hF gene

Activation and Purification
Expression ofrF in culture medium
BHK cells
hF human factor
BHK baby hamster kidney
11
Recombinant Factors

Advantages
Safe and stable source of the agent
When sources are scarce
Problems
Contaminating proteins Infectious or immunogenic
agent
Expensive

12
Genetic Study

Study the development of inhibitors.
Gene Transfer Sustained therapeutic production
of factors with No stimulation of an immune
response .

13
The Tools of Genetic Engineering

DNA gene fragment of interest
Endonucleases
Plasmid
Ligase
Host that is capable of accepting DNA
Insertion into the genetic machinery
Confirm that the gene is inserted.
Purify the protein of interest

14
Gene Transfer Clinical Trials

5 trials approved in the States .
Retroviral vector B-domain deletion
Non-viral approach reduction factor use
spontaneous bleeding episodes.
Gutless adenovirus eliminate immune response

15
Results Of Clinical Trials

Long-term therapeutic expression not achieved,
but data are encouraging.
Detectable factor levels observed.
The subjective decreased bleeding .
No evidence of inhibitor.
Hepatic toxicity , thrombocytopenia.
Decline expression .

16
Shortcoming Of Treatment Modalities

Short T 1/2
Coast
Infections Immunologic
Hepatic toxicity ,low platelets
Decline expression.
Owing to the shortcoming of treatment Modalities
prompted the need for anew hemostatic agent.

17
Initiation of Haemostasis
prothrombin
X
VIII/vWF
VIIIa
VIIa
TF
Xa
V
Va
thrombin
Va
TF-bearing cell
XI
XIa
VIIa
IX
Fibrinogen
platelet
prothrombin
IXa
X X
XIa
thrombin
Fibrin
IXa
VIIIa
Xa
Va
activated platelet
IX
18

TFindependent mechanism of rFVIIa enhanced
hemostasis

19
Rational

Thrombin crucial role in haemostasis.
Any agent that enhances the thrombin generation
'general haemostatic agent'.
rFVII enhances thrombin generation on activated
platelets
Compensates for lack of FVIII and FIX.
Normalize fibrin clot permeability

20
Pharmacokinetic

t½ 2.7 h
Inter-subject variability.
Rapid clearance in children gt adults.
No readily available assays
The haemostatic levels remains uncertain.
Frequent bolus injections, IVI potential to
minimize usage.

21
Potential Use

Increases thrombin generation on activated
platelet
Hemophilia (FVIII/FIX deficiency)
Acquired hemophilia.
Platelet disorders qualitative and quantitative
Diffuse bleeding triggered by surgery and trauma.
Impaired initial hemostasis
FVII-deficiency
Liver disease
Oral anticoagulant therapy

22
Hemophilia with inhibitors

FDA Approved Feb 1999
Bleeding during or prior to ITI therapy.
Control bleeding during surgery.
Safe and effective in 92 hemophilia research
society registry
Inhibitor titres are not boosted.
Home treatment mild-moderate episodes.
Recommended dose 60-120 ug/kg q 2 -6 h or IVI.

23
Acquired Hemophilia

Rare but potentially life-threatening condition
mortality rate 20.
Auto-antibodies against the deficient factor.
rFVIIa is effective in major bleeding
Induces haemostasis independent of the presence
of FVIII or FIX.
Well tolerated in these patients

24
Liver Disease

Reduction in the synthesis of factors involved in
coagulation and fibrinolysis.
Moderate thrombocytopenia.
Upper gastrointestinal tract.
Vitamin K .
FFP
PCCs thromboembolic complications.

25
rFVII Liver Disease

Acute hepatic trauma, liver biopsy, chronic
liver disease ,cirrhosis, and liver
transplantation.
Experimental studies seems to be safe and
effective.
No evidence of thrombosis .
Cirrhosis , achieved hemostasis in 74
Jeffers et al

26
The Risk Of Thrombosis In LIVER Patients

No evidence of dose relationship
Many events have an alternative aetiology
Few events within the first day after dosing
No increase in events as compared with background
transplant population

27
Drug-Induced Coagulopathy

Oral anticoagulant treatment ? hemorrhage 0.6/
m .
Vitamin K, FFP or PCCs
rFVIIa in healthy volunteers 50 drop of INR
Girard et al
An open, multicenter pilot trial is underway to
determine the efficacy
Fondaparinux. normalized PT, aPTT, and TT.
Bijsterveld et al

28
Glanzmanns Thrombasthenia

Refractory to platelet transfusion
Increases the initial thrombin generation,
thereby compensating for defective platelet
Effective in 60 during surgery .
No adverse effects of rFVIIa
International registry data relatively safe and
effective when used in GT.
Blood 1999 94 (11)
3951-3953

29
Thrombocytopenia

Increased thrombin generation on activated
platelets compensate for the low platelet number.
Reduction in bleeding time in 52.4 of 105
patients .
Kristensen et al
No major adverse

30
Surgical Trauma patients

Effective and safe in the management of
uncontrolled surgical in patients not known to
have inherited coagulopathy.
Trauma surgical intervention failed to stop
life- threatening bleeding.
Significant decrease to 2 packed RBC
Shortening of PT aPTT
Adjunctive hemostatic treatment
Theoretical risk of TED ,none observed

31
Building Strong Scientific Evidence