Immune Thrombocytopaenia (ITP)

Article Last Updated:20/03/2026

Important clarification in terminology:

The term idiopathic thrombocytopaenic purpura is now outdated
ITP is currently defined as immune thrombocytopaenia, reflecting its underlying autoimmune mechanism rather than an unknown (“idiopathic”) cause

ITP is therefore classified as:

Primary ITP: no identifiable underlying cause
Secondary ITP: associated with an underlying condition

Definition

ITP is an acquired immune-mediated disorder characterised by isolated thrombocytopaenia, and is a diagnosis of exclusion (i.e. no alternative non-immune cause identified).

Epidemiology

ITP affects both children and adults ^[Ref]

Children: usually acute and self-limiting
Adults: more likely to develop chronic ITP

Aetiology

ITP may be classified as primary or secondary, and is a diagnosis of exclusion of non-immune causes of thrombocytopaenia. ^[Ref]

Primary ITP

No identifiable underlying cause – most common form

Secondary ITP

Associated with an underlying condition, including:

Drugs (drug-induced)
Infection (e.g. HIV, hepatitis B and C, CMV, EBV)
Lymphoproliferative disorders (e.g. CLL, Hodgkin’s lymphoma)
Immunodeficiency syndrome
Other autoimmune diseases (e.g. SLE, RA, APS)
Evans syndrome (ITP + autoimmune haemolytic anaemia)

The exact pathophysiology is complex and incompletely understood. ^[Ref]

As a general concept, antibody-coated platelets are prematurely destroyed in the spleen and/or liver. ^[Ref]

Clinical Features

Clinical features of ITP are highly variable and depend on the degree of thrombocytopaenia ^[Ref1]^[Ref2]

Many patients are asymptomatic and are diagnosed incidentally
If symptomatic, ITP presents with isolated thrombocytopaenia
- Classic mucocutaneous bleeding (e.g. petechiae, epistaxis, gum bleeding, menorrhagia)
- Severe haemorrhage (e.g. GI bleeding, intracranial haemorrhage) is less common and usually happens if platelet counts are very low
- The patient is usually otherwise well with normal examination findings apart from bleeding signs (i.e. no splenomegaly, no lymphadenopathy etc.)

Differential Diagnosis

ITP is a diagnosis of exclusion, therefore other causes of thrombocytopenia must be considered: ^[Ref]

Differential diagnosis	Key suggestive features
TTP	MAHA + thrombocytopaenia (key features) +/- Renal impairment, fever, neurological features ↓ ADAMTS13 levels Direct Coombs test -ve haemolytic anaemia See the Thrombotic Thrombocytopaenic Purpura (TTP) article for more information
Heparin-induced thrombocytopaenia	Recent heparin exposure Thrombocytopaenia + paradoxical thrombosis Investigation: platelet factor 4-heparin antibody test
Aplastic anaemia	Pancytopaenias Hypocellular bone marrow
Acute leukaemias	Other cytopaenis Abnormal peripheral blood smear and bone marrow analysis See the Acute Leukaemia article for more information
Myelodysplastic syndrome	Cytopenias (often multiple) Dysplastic cells on blood film

Investigation and Diagnosis

ITP is a diagnosis of exclusion, characterised by: ^[Ref]

Isolated thrombocytopenia (platelet count <100 × 10⁹/L) – low platelets with otherwise normal blood counts and blood film
With no alternative cause identified (see the differential diagnosis section above)

Initial tests to exclude alternative causes:

FBC → to confirm isolated thrombocytopaenia
Peripheral blood film → exclude TTP (schistocytes) and leukaemias (blasts)
Coagulation screen → exclude DIC
Viral screen (e.g. HIV, hepatitis B and C) → identify secondary causes
Autoimmune screen → identify secondary causes

Management

Management depends on bleeding severity, platelet count, and individual risk factors.

Do not routinely offer prophylactic platelet transfusions in ITP.

Platelet transfusions should only be used in active / significant bleeding and must be given with immunosuppression, as transfused platelets are rapidly destroyed.

Acute Management

Acute management is indicated in: ^[Ref]

Active significant or life-threatening bleeding, or
Very low platelet count (<10 x 10⁹/L)

Acute management components: ^[Ref]

Immediate measure	Stop any anticoagulants / antiplatelets if possible
Core treatment	IV corticosteroids IV immunoglobulin Platelet transfusion – provides a transient increase in platelet count, must not be used alone (combine with steroids and immunoglobulin therapy)
Adjuncts	Tranexamic acid can be added to stop life-threatening bleeding, esp. for mucosal bleeding

Long-Term Management

Active observation (no treatment) is appropriate in patients who are asymptomatic or have only mild mucocutaneous bleeding. ^[Ref]

In children, ITP is often acute and self-limiting → observation under the supervision of a haematologist is often appropriate. ^[Ref]

Treatment is generally initiated to prevent future bleeding if: ^[Ref]

Platelet count <20-30 x 10⁹/L – common criteria
High-risk features (e.g. >65 y/o, history of bleeding, concurrent use of anticoagulants / antiplatelets, renal impairment)

Choice of treatment: ^[Ref]

1st line: oral corticosteroids (usually prednisolone or dexamethasone)
Further therapy:
- Thrombopoietin receptor agonists (e.g. avatrombopag, eltrombopag, romiplostim)
- Fostamatinib
- Rituximab
Splenectomy – to be considered if refractory to drugs (most effective treatment)

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