sticky blood syndrome

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sticky blood syndrome

This

syndrome was first described in 1983-1986 as the association of arterial and

venous thrombosis with antibodies directed against phospholipids.

Originally

noted as a complication in approximately 30% of patients with systemic lupus erythematosus, it is now also diagnosed in patients with thrombotic episodes and anti-phospholipid

antibodies (aPL) but without

clinical features of SLE - primary antiphospholipid

syndrome.

aetiology

There is

a familial association in some cases of APS. HLA studies suggest DR7, DR4 and

DQw7 plus DRw53 are risk factors.

The aPL antibody is targeted to the

combination of cardiolipin with a plasma protein

called beta-glycoprotein I.

In vivo aPL has a procoagulant

effect on:

platelet membranes

endothelium

prothrombin,

protein C and protein S

aPL is found in the serum

of 30% of patients with SLE, in this context it is termed " lupus

anticoagulant " .

lupus anticoagulant

The lupus

anticoagulant is an immunoglobulin, IgG or IgM, which binds to phospholipids and prevents coagulation

reactions from taking place on the platelet surface.

It is

associated with arterial and venous thrombosis, and recurrent spontaneous

abortions. It occurs in about 30% of patients with systemic lupus erythematosus but may be found in other autoimmune

diseases, in response to drugs such as phenothiazine,

and in patients with infectious diseases such as AIDS. Often, no underlying

condition may be found.

The LA

anti-phospholipid often occurs in association with

anti-cardiolipin antibodies (aCL)

- 59% of patients with SLE having LA also have aCL,

and 45% with SLE and aCL, also have LA.

detection of lupus coagulant

There is

no direct test for the lupus anticoagulant (LA). Detection is based upon its

inhibitory actions on coagulation. It binds to phospholipid

on the platelet surface and interferes with the formation of the prothrombin activator complex.

Clotting

times are increased and are not corrected by the dilution with normal plasma:

increased activated

partial thromboplastin time

increased prothrombin time

There is

a false positive VDRL test.

Lupus

anticoagulant should be suspected whenever there is a markedly prolonged PTT

without clinical bleeding.

In SLE,

the lupus anticoagulant is usually noted in patients who present with stroke, thrombophlebitis, and renal vein or mesenteric artery

thrombosis.

detection of anticardiolipin antibodies

The

earlier VDRL test using cardiolipin as antigen is

insensitive. Modern procedures use solid-phase radioimmunoassay - RIA - or

enzyme linked immunoabsorbent assay - ELISA. Since

1990, reporting of results have been standardised and

are expressed in terms of GPL or MPL units.

The risk

of thrombosis or spontaneous abortion increases with the titre

of aCL and are greater with IgG

antibodies than with IgM - for example, of 39

patients with IgG greater than 20 GPL units, 70% had

a thrombotic event.

epidemiology

the

diagnosis of antiphospholipid syndrome requires

that a patient have recurrent clinical events (such as thromboses or fetal

loss) and an antiphospholipid antibody (such as anticardiolipin antibody or lupus anticoagulant).

about

50% of patients with antiphospholipid syndrome

have the primary form of the disease.

about

1/3 of patients with SLE have antiphospholipid

antibodies but not all of those have the syndrome.

in

about 2% of the normal population, detectable antiphospholipid

antibodies are present. In 0.2% the titre is

high.

the

clinical course and severity of the lupus is worsened by the presence of

the antiphospholipid syndrome.

the

annual risk of thrombosis in untreated patients is 1 in 3 per year.

clinical features

The

clinical features are presented according to the systems affected:

neurological

cardiac

renal

endocrine

dermatological

haematological

obstetric

thrombotic

neurological

Thrombosis

causes ischaemic damage to the brain. MRI scans show

a wide range of brain infarcts - single or multiple, large or small.

Repeated

episodes may result in dementia.

Migraine

is common and may be the first symptom.

Epilepsy

and chorea are associated.

Transverse

myelopathy is a rare, but specific, association.

stroke

A stroke

is a focal neurological deficit, secondary to a vascular lesion,

that lasts for longer than 24 hours.

Strokes

result from:

cerebral

infarction (84%):

secondary to

thrombosis (53%); or

embolus

(31%)

primary

intracerebral haemorrhage

(10%)

subarachnoid haemorrhage

(6%)

The

definition of stroke excludes transient ischaemic

attacks, subdural haematomas,

and infarction or haemorrhage due to infection or tumour. However, practically it is often difficult to

discriminate between a small stroke and a transient ischaemic

attack.

transient ischaemic attacks

Transient

ischaemic attacks are focal CNS disturbances caused

by vascular events such as microemboli and occlusion

leading to ischaemia where the symptoms last less

than 24 hours and there are no permanent neurological sequelae.

Transient

ischaemic attacks are a risk factor for subsequent

stroke or myocardial infarction.

Diagnosis

rests critically upon the patient's history since the attacks are seldom

witnessed by a physician and there are no confirmatory tests.

Emboli

are the major cause.

haematological

thrombocytopenia -

30% of patients with idiopathic thrombocytopenic purpura

have aPL

autoimmune haemolytic anaemia - this is

a rare feature

thrombocytopaenia

Thrombocytopaenia is a decrease

in the number of platelets in the blood - it reduces the ability of the blood

to clot and is thus a bleeding diathesis. It is defined as a platelet count

less than 100,000 per cubic ml.

In

addition, it is important to consider also the causes of apparent thrombocytopaenia - i.e. conditions where there is platelet

dysfunction.

Neonatal thrombocytopaenia has a modified differential diagnosis.

thrombotic

Venous:

DVTs

- these may be recurrent. In women these may appear appear

to be triggered by the use of the oral contraceptive pill

hepatic

thrombosis - antiphospholipid syndrome is the

second most common cause of antiphospholipid

syndrome.

retinal vein

thrombosis

renal vein

thrombosis

major vein

thrombosis may involve thoracic outlet veins or the inferior vena cava

Arterial

thrombosis may cause ischaemia of almost any organ

pulmonary hypertension

Pulmonary

hypertension is of two types:

pulmonary artery

hypertension:

this results from

disorders of the lung or arterial vasculature

pulmonary venous

hypertension:

this results from

disorders of the pulmonary venous drainage or of the left heart

detection of lupus coagulant

There is

no direct test for the lupus anticoagulant (LA). Detection is based upon its

inhibitory actions on coagulation. It binds to phospholipid

on the platelet surface and interferes with the formation of the prothrombin activator complex.

Clotting

times are increased and are not corrected by the dilution with normal plasma:

increased activated

partial thromboplastin time

increased prothrombin time

There is

a false positive VDRL test.

Lupus

anticoagulant should be suspected whenever there is a markedly prolonged PTT

without clinical bleeding.

In SLE,

the lupus anticoagulant is usually noted in patients who present with stroke, thrombophlebitis, and renal vein or mesenteric artery

thrombosis.

detection of anticardiolipin antibodies

The

earlier VDRL test using cardiolipin as antigen is

insensitive. Modern procedures use solid-phase radioimmunoassay - RIA - or enzyme

linked immunoabsorbent assay - ELISA. Since 1990,

reporting of results have been standardised and are

expressed in terms of GPL or MPL units.

The risk

of thrombosis or spontaneous abortion increases with the titre

of aCL and are greater with IgG

antibodies than with IgM - for example, of 39

patients with IgG greater than 20 GPL units, 70% had

a thrombotic event.

treatment

Identification

of this syndrome means that many patients who were in the past diagnosed as

suffering from a 'vasculitis' and treated with

anti-inflammatory regimes and high-dose corticosteroids, will, if found to be

suffering from APS, respond better to anticoagulation therapy:

first-line treatment

is low dose aspirin - 75-100 mg daily (1)

patients

with APS who have had a documented major thrombotic

event require long-term treatment with warfarin

or coumarin anticoagulation. An international

normalized ratio of 3.0 or higher is required. The risk that warfarin treatment will result in haemorrhage

is 1 in 14 per year (the risk of serious haemorrhage

is 1 in 50 per year) - this compares favorably with the annual risk of 1

in 3 for new thrombosis in untreated patients and 1 in 5 in patients

treated with aspirin alone or lower doses of warfarin.

prognosis

a high lifetime risk

of thrombosis is conferred by the presence of antiphospholipid

antibodies in the blood

of 'young' people

who suffer strokes, up to 20% of them have antiphospholipid

syndrome

up to 20% of cases

of recurrent miscarriage have antiphospholipid

syndrome

up to 20% of cases

of DVT have antiphospholipid syndrome

there is a

possibility that the antibodies directed against phospholipids, such as

those found in antiphospholipid syndrome, may

have a causative role in the development of atheroma

Much

Love,

Deanna

LUPUS

Serenity Prayer...

Lord, grant me the

serenity to accept the things I cannot change, the courage to change the things

I can, and the wisdom to hide the bodies of doctors I shot when they said,

You're perfectly healthy, it's all in your head "