Bernard soulier syndrome

Bernard-Soulier Syndrome
An Inherited Platelet Disorder

• Bernard-Soulier syndrome (BSS) was first
recognized in 1948 by two French
hematologists—Jean Bernard and Jean Pierre
Soulier.
• They described a patient from a
consanguineous family afflicted with severe
bleeding episodes, thrombocytopenia, and
very large platelets.

• Heterozygous carriers are usually asymptomatic,
although they may have mild bleeding
tendencies.
• It has an autosomal recessive mode of
inheritance
• There have also been reports of a mild form of
BSS with an autosomal dominant inheritance
trait.

PATHOPHYSIOLOGY
• Platelets play a critical role in normal primary
hemostasis and clot formation.
• The platelet membrane contains specific
glycoprotein (GP) receptors, which function in
platelet adhesion, activation, and aggregation.
• The GPIb-IX-V receptor complex, is responsible
for platelet adhesion through its interaction with
von Willebrand factor on the exposed
subendothelium,.

• It is composed of 4 transmembrane
polypeptide subunits—disulfide-linked alpha
and beta subunits of GPIb, and non covalently
bound subunits GPIX and GPV.
• The platelets of BSS lack or have a
dysfunctional GPIb-IX-V receptor resulting in
defective adhesion to the subendothelium.

• The dysfunctional platelets found in BSS can
result from one of several different glycoprotein
mutations such as missense, nonsense, or
deletion mutations of the GPIb-α, GPIb-β, or
GPIX genes.
• This variety of mutations is most likely
responsible for the heterogeneity of BSS.

CLINICAL MANIFESTATIONS
• Bernard-Soulier syndrome presents early with
bleeding symptoms, most commonly
– epistaxis
– ecchymosis
– cutaneous and gingival bleeding,
– menometrorrhagia
– gastrointestinal bleeding.
• Rarely, patients will have severe hemorrhage
at times of injury or surgery.

• The severity of these bleeding symptoms is
variable among patients and may range from
mild to life-threatening.
• Heterozygous patients may have mild to
moderate bleeding tendencies.

LABORATORY FINDINGS
• Thrombocytopenia is variable in BSS, and the
platelet count typically ranges from less than
30 to 200 x 103/L.
• Bleeding times may range from marginal to
markedly prolonged

• Peripheral blood smear will reveal large
platelets
– Typically more than one third of the platelets are
about half of the size of a red blood cell (3.5
micrometre)
– Some platelets are as large or larger than a
lymphocyte
• Bone marrow biopsy - normal numbers of
megakaryocytes without significant
morphologic abnormalities

• Modern platelet function tests, such as the
PFA-100, may be useful but with variable
sensitivity, depending on the severity of the
defect.
• Currently, their use is limited to screening for
platelet dysfunction, and further testing, such
as aggregometry or flow cytometry, is
necessary for confirmation.

• In vitro platelet aggregation studies
characteristically show a failure to aggregate
with ristocetin and slow response with low
doses of thrombin
• This failure to aggregate cannot be corrected
with the addition of normal plasma, which
distinguishes BSS from vonWillebrand disease.

• The platelets show normal aggregation
– Epinephrine
– Adenosine diphosphate
– Collagen, and
– Arachidonic acid.

• Flow cytometry can be used to confirm
defects in the GPIb-IX-V complex by antibodies
directed against platelet surface antigen
CD42b, revealing a severe reduction or
deficiency of GPIb .
• Other platelet antigens, CD41 (GPIIb) and
CD61 (GPIIIa), are normal

• The cause of thrombocytopenia in BSS is
unknown, and early studies suggested
decreased platelet survival.
• However, a later study using 111indium-oxine
labeled platelets shows little or no decrease in
platelet survival time, suggesting ineffective or
decreased thrombopoiesis.

DIFFERENTIAL DIAGNOSIS
• Inherited giant platelet disorders
– May-Hegglin anomaly and
– Other MYH9-related thrombocytopenia syndromes
(Fetchtner syndrome, Sebastian syndrome, and Epstein
syndrome)
• characterized by
– giant platelets,
– autosomal dominant inheritance trait, and
– mutations of the MYH9 gene on chromosome 22q12-13,
which is the gene encoding for the heavy chain of
nonmuscle myosin IIA (NMMHC-IIA).

May-Hegglin anomaly
• Most common inherited giant platelet
disorder and has a clinical manifestation much
like that of BSS with mild bleeding tendencies.
• These patients will often have other clinical
findings including nephritis, familial spastic
paraplegia, and pituitary growth hormone
deficiency.

• In vitro platelet aggregation tests show normal
response to adenosine diphosphate, collagen,
epinephrine, and ristocetin; however, impaired
response to epinephrine has been described
• Peripheral smear evaluation shows large platelets
and Dohle bodies, a blue spindle-shaped
inclusion, within the cytoplasm of neutrophils

Gray platelet syndrome
• Extremely rare giant platelet disorder
• Autosomal dominant mode of inheritance as well as
some seemingly sporadic cases.
• Patients tend to present early with epistaxis,
ecchymosis, and other bleeding symptoms.
• Thrombocytopenia is common; however, bleeding time
is prolonged even in patients with normal platelet
counts, suggesting a qualitative platelet disorder

• Platelet aggregometry shows reduced response to
collagen and thrombin, but normal responses to
adenosine diphosphate and arachidonic acid.
• Ristocetin may have normal or reduced, but not
absent, response.
• The peripheral blood smear reveals large agranular
platelets that appear gray-blue on Wright-Giemsa stain.
• The bone marrow biopsy specimen usually shows
normal megakaryocytes and reticulin fibrosis

von Willebrand disease
• Most commoninherited bleeding disorder,
may present with symptoms - mucocutaneous
bleeding, epistaxis,and ecchymosis.
• Not typically associated with
thrombocytopenia or significant peripheral
smear findings.

• Platelet aggregation tests show failure to
aggregate in the presence of ristocetin, much
like BSS.
• However, a ristocetin cofactor activity test,
using the patient’s plasma and freshly washed
platelets to measure the von Willebrand factor
activity in the plasma will be reduced in
patients with von Willebrand disease

Immune thrombocytopenic purpura
• Caused by antiplatelet antibodies, leading to the
accelerated destruction of platelets.
• Peripheral smear evaluation - decreased platelets,
• Bone marrow evaluation will show normal or increased
numbers of megakaryocytes.
• The diagnosis of immune thrombocytopenic purpura
requires the exclusion of other causes of
thrombocytopenia

• Possible causes of immune thrombocytopenia
include infections, autoimmune diseases,
lymphoproliferative diseases and drug therapy

• Immune thrombocytopenic purpura can be
separated into childhood and adult types.
• Childhood immune thrombocytopenic purpura is
typically acute onset, often develops after viral
infection or vaccination, and is frequently self-
limited with resolution in weeks to months
• Adult type is usually a chronic disease with
insidious onset, more often involves women, and
rarely resolves spontaneously

TREATMENT
• Platelet and/or blood transfusions remain the
best therapeutic measure for uncontrolled
bleeding and prophylaxis to control bleeding
during surgery.
• The benefits of receiving the transfusions must
be weighed against the risks of exposure.
• Repeated exposure to blood products raises
concern for alloimmunization and platelet
refractoriness

• The use of leukoreduced blood components
has been shown to decrease alloimmune
platelet refractoriness.
• Although some authors have suggested that
patients should receive platelets from human
leukocyte antigen–matched donors in order to
avoid alloimmunization, currently this is not a
widely accepted strategy.

• Activated factor VIIa (FVIIa) has been reported
to reduce bleeding times in patients with BSS.
• However, FVIIa is an experimental drug in
treatment of inherited thrombocytopenia, and
adverse reactions have been reported.

• Desmopressin, a synthetic analog of antidiuretic
hormone, may transiently increase factor VIII and von
Willebrand factor by causing their release into blood.
• It is used for treatment of mild hemophilia A and von
Willebrand disease.
• Desmopressin has been reported to shorten bleeding
episodes for some patients, but a test dose is
recommended to determine those patients who will
benefit

• Stem cell transplantation has been
successfully used to treat children with BSS
who had severe, life-threatening bleeding
episodes; however, based on the study results,
the use of transplantation should only be
considered in severe disorders and after
patients have developed antiplatelet
antibodies

• Patients with BSS should be counseled about
the importance of preventing even minor
trauma as well as avoiding aspirin containing
medications and other platelet antagonists

CONCLUSION
• Bernard-Soulier syndrome is one of several inherited giant
platelet disorders distinguished by a functional abnormality of
the GPIb-IX-V platelet GP receptor complex.
• The disease is highly variable with bleeding tendencies that
can range from mild to severe and life-threatening.
• Platelet aggregation studies and, more definitively, flow
cytometry can provide an accurate diagnosis of this rare
disease and allow for adequate therapeutic management

Bernard soulier syndrome

More Related Content

What's hot

Viewers also liked

Similar to Bernard soulier syndrome

More from Shahin Hameed

Recently uploaded

In this document

Bernard soulier syndrome