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Polycythaemia Vera

BSH Diagnosis and management of polycythaemia vera. Date: Nov 2018.

Article Last Updated:17/03/2026

Definition

Essential thrombocythaemia is a MPN characterised by clonal proliferation of haematopoietic stem cells in the bone marrow, resulting in:

  • Increased red cell mass (erythrocytosis)
  • Often with concurrent leucocytosis and thrombocytosis

MPNs are a group of clonal haematopoietic stem cell disorders characterised by overproduction of mature myeloid lineage cells. The 4 classical myeloproliferative neoplasms are:

  • Primary myelofibrosis
  • Polycythaemia vera
  • Essential thrombocythaemia
  • Chronic myeloid leukaemia

MPNs share several features:

  • Mutations affecting the JAK-STAT signalling pathway (most commonly JAK2, but also CALR or MPL mutations)
    • CML is distinct, driven by the Philadelphia chromosome (BCR-ABL fusion gene)
  • Bone marrow hypercellularity
  • ↑ Risk of thrombosis (particularly in polycythaemia vera and essential thrombocythaemia)
  • Risk of transformation to AML

Aetiology

Almost always caused by JAK2 mutation

  • JAK2 V617F mutation is found in >95% of patients with polycythemia vera
  • JAK2 exon 12 mutations are found in most remaining cases

The mutation causes constitutive activation of the JAK-STAT signalling pathway → EPO-independent RBC production

JAK-2 negative polycythaemia vera is a very rare clinical entity.

Clinical Features

Typically presents at a median age of 60 y/o

Cutaneous features
  • Pruritus – hallmark feature
    • Often described as excruciating
    • Aquagenic pruritus is classic – pruritus triggered / worsened by contact with hot water (e.g. after a bath)
  • Facial plethora
Microvascular disturbances Due to hyperviscosity

  • Erythromelalgia (burning pain, warmth, and redness of the hands or feet)
  • Headache
  • Visual disturbance
Thrombotic complications
  • DVT / PE
  • Unusual site thrombosis (e.g. portal vein thrombosis, Budd-Chiari syndrome)
  • Arterial thrombosis (e.g. ischaemic stroke, myocardial infarction)
Other features
  • Splenomegaly (typically mild, not like massive splenomegaly seen in primary myelofibrosis and CML)
  • Constitutional symptoms (e.g. fatigue, night sweats, weight loss)

Due to the high turnover of cells and associated hyperuricaemia, gout may be present at diagnosis.

Investigation and Diagnosis

Test Typical findings
FBC
  • Haematocrit (>0.52 in men and >0.48 in women)
  • Often with concurrent
    • Leucocytosis
    • Thrombocytosis
Red cell mass study
  • ↑ Red cell mass (>25% above the predicted mean)
Biochemistry
  • ↓ Serum EPO (or inappropriately normal)
  • ↓ Serum ferritin (as excessive RBC production consumes iron stores)
  • LDH
Molecular testing
  • JAK2 V617F mutation (>95% cases)
  • JAK2 exon 12 mutations (most remaining cases)
Bone marrow biopsy Typical findings

  • Hypercellularity with trilineage expansion (bone marrow panmyelosis)
  • Pleomorphic megakaryocyte clusters

Disclaimer:

No formal diagnostic criteria are included in this section. This is because the diagnostic criteria outlined in the 2018 BSH guideline are now considered outdated and have been replaced by more recent classification frameworks. These newer frameworks (e.g. WHO 2022 and ICC 2022) broadly incorporate many of the key findings listed above.

For UKMLA and non-specialist level learning, it is more important to recognise these key findings than to learn specific diagnostic criteria.

Management

1st Line Therapy – All Patients

The following should be offered to ALL patients, regardless of their risk category:

  • Venesection – to maintain a target haematocrit of <0.45
  • Low-dose aspirin (75-100 mg daily)
  • Cardiovascular risk management (e.g. smoking cessation, treating hypertension / diabetes / hyperlipidaemia)

Cytoreductive Therapy – Selected Patients

Indications:

  • High-risk patients (≥65 y/o or history of polycythaemia-associated thrombosis)
  • Low-risk patients with
    • Persistent leucocytosis
    • Extreme / progressive thrombocytosis (≥1500 x 109/L)
    • Venesection not tolerated / unable to control haematocrit
    • Progressive / symptomatic splenomegaly
    • Uncontrolled disease-related symptoms (e.g. weight loss, night sweats)

Choice of cytoreductive therapy:

  • Hydroxycarbamide, or
  • Interferon-alpha

Differential Diagnosis

Secondary Polycythaemia

Definition

Secondary polycythaemia refers to erythrocytosis caused by increased EPO production, typically in response to chronic hypoxia or pathological EPO secretion.

This contrasts with polycythaemia vera, which is a primary MPN characterised by autonomous red blood cell production that occurs independently of EPO regulation.

Aetiology

Category Common causes
Central hypoxia
  • Chronic lung disease (e.g. COPD)
  • Carbon monoxide exposure (e.g. chronic smokers, occupational exposure)
  • Cyanotic heart disease (right-to-left shunting)
  • Sleep apnoea
  • High altitude
Renal (local) hypoxia
  • Renal artery stenosis
  • Mass effect (e.g. hydronephrosis, renal cysts, polycystic kidney disease)
Pathological EPO production
  • Renal cell cancer (classic)
  • Hepatocellular carcinoma
  • Cerebellar haemangioblastoma
Drug induced
  • Exogenous EPO
  • Testosterone / anabolic steroids (e.g. performance-enhancing drugs used in bodybuilding)

Polycythaemia Vera vs Secondary Polycythaemia

Key factors that differentiate between polycythaemia vera and secondary polycythaemia

Feature Polycythaemia vera Secondary polycythaemia
Serum EPO Low (or inappropriately normal) High
White cell and platelet count Often elevated Normal
Oxygen saturation Normal May be low (in hypoxia-driven causes)
Splenomegaly Common Uncommon
JAK2 mutation Present Absent
Bone marrow biopsy Hypercellular with trilineage expansion (panmyelosis) Isolated erythroid proliferation

Relative Polycythaemia

Definition

Relative polycythaemia refers to an apparent increase in haemoglobin and haematocrit due to reduced plasma volume, in the presence of a normal red cell mass.

In contrast, true polycythaemia refers to an absolute increase in red cell mass, and includes both polycythaemia vera and secondary polycythaemia.

Aetiology

Relative polycythaemia is caused by plasma volume depletion, rather than increased erythropoiesis.

Common causes include: [Ref]

  • Dehydration – most common
  • Gaisbock syndrome (stress polycythaemia) – haemaoconcentration associated with
    • Diuretic use
    • Smoking
    • Obesity
    • Hypertension

Clinical Features

Relative polycythemia is NOT associated with the clinical features of true polycythemia, such as pruritus, leukocytosis, or thrombocytosis. [Ref]

It does NOT carry the same thrombotic risk.

True vs Relative Polycythaemia

True polycythaemia includes both polycythaemia vera and secondary polycythaemia. Characterised by an absolute increase in red cell mass. [Ref1][Ref2]

Feature True polycythaemia Relative polycythaemia
Red cell mass Increased Normal
Haematocrit Increased
Haemoglobin

Relative polycythaemia reflects haemoconcentration, whereas true polycythaemia reflects increased red cell mass.

References

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