Haem: CML and myeloproliferative disorders

Question 1

What is polycythaemia?

Answer 1

A condition characterised by raised Hb concentration and raised haematocrit.

Question 2

What are the two main types of polycythaemia?

Answer 2

Relative - caused by a lack of plasma (associated with alcoholism, obesity and diuretics)

True - caused by an excess of erythrocytes

Question 3

What is secondary polycythaemia and what can cause it?

Answer 3

• Polycythaemia that occurs due to excessive stimulation by EPO (there is no problem with the bone marrow itself)
• Appropriate causes: high altitude, hypoxic lung disease, cyanotic heart disease, high affinity haemoglobin
• Inappropriate causes: renal disease (cysts, tumours), uterine myoma, other tumours

Question 4

How can myeloproliferative neoplasms be broadly categorised?

Answer 4

• Philadelphia positive: CML
• Philadelphia negative: polycythaemia vera, essential thrombocythaemia, primary myelofibrosis

Question 5

What are the two processes that cell undergo as they develop and how are these different in acute and chronic leukaemia?

Answer 5

• Two processes: differentiatoin + proliferation
• Chronic leukaemia: differentiation is intact (produces mature cells) + proliferation is excessive and abnormal
• Acute leukaemia: differentiation is abnormal (cells have lost the ability to mature) + proliferation is excessive and abnormal

Question 6

What are the main types of myeloid malignancy?

Answer 6

• Acute myeloid leukaemia (blasts >20%)
• Chronic myeloid leukaemia
• Myeloproliferative disorders
• Myelodysplastic syndromes (blasts 5-19%)

Question 7

Mutations in which genes are commonly associated with the development of myeloproliferative disorders?

Answer 7

Tyrosine kinase

Question 8

What is the normal physiological role of tyrosine kinase?

Answer 8

• Transmit cell growth signals from cell surface receptors to the nucleus
• They are activated by transferring phosphate groups to itself and downstream proteins
• They promote cell growth but they do NOT affect maturation

Question 9

Name three genes that are associated with myeloproliferative disorders.

Answer 9

• JAK2 (V617F)
• Calreticulin
• MPL

Question 10

Which conditions is defined by the presence of one of these mutations?

Answer 10

100% of polycythaemia vera has JAK2 V617F mutation

NOTE: it is also found in 60% of primary myelofibrosis and essential thrombocythaemia

Question 11

What is the normal physiological role of JAK2? How is this different in polycythaemia vera?

Answer 11

• It is a tyrosine kinase that is normally bound to the inactive EPO receptor. When EPO binds to the receptor, the receptor dimersises, autophosphorylates and phosphorylates JA2 which promotes cell proliferation.
• Mutated JAK2 is constitutively active in the absence of EPO thereby driving cell replication in the absence of a stimulus.

Question 12

What is the diagnosis of myeloproliferative disorders based on?

Answer 12

• Clinical features (splenomegaly is particularly important)
• FBC
• Bone marrow biopsy
• EPO level
• Mutation testing

Question 13

Outline the typical presentation of polycythaemia vera?

Answer 13

• Often incidental
• Hyperviscosity: headaches, visual disturbance, stroke, fatigue, dyspnoea, light-headedness
• Increased histamine release: aquagenic pruritis, peptic ulceration

Question 14

Outline the principles of treatment of polycythaemia vera.

Answer 14

• Reduce haematocrit (aim for <45%) - venesection, cytoreductive therapy (hydroxycarbamide)
• Reduce thrombosis risk - control Hct, aspirin, keep platelets < 400x10⁹/L

Question 15

What is essential thrombocythaemia?

Answer 15

Chronic myeloproliferative disorder mainly involving the megakaryocyte lineage

Characterised by sustained thrombocytosis > 600 x10⁹/L

Question 16

Outline the typical presentation of essential thrombocythaemia.

Answer 16

• Incidental finding (50%)
• Thrombosis (arterial and venous) - CVA, TIA, DVT, PE, gangrene
• Bleeding (mucous membrane and cutaneous)
• Headaches, dizziness, visual disturbance
• Splenomegaly (modest)

NOTE: ET can cause both thrombosis and bleeding depending on the way in which the abnormal platelet function

Question 17

Outline the treatment options for essential thrombocythaemia.

Answer 17

• Aspirin
• Hydroxycarbamide
• Anagrelide (specifically inhibits platelet function but rarely used because of side-effects)

NOTE: hydroxycarbamide is an antimetabolite that suppresses cell turnover

Question 18

Outline the prognosis for essential thrombocythaemia.

Answer 18

• Normal life span in many patients
• 5% in 10 years risk of leukaemic transformation
• Myelofibrosis is uncommon

Question 19

What is primary myelofibrosis?

Answer 19

• A clonal myeloproliferative disease associated with reactive bone marrow fibrosis
• Characterised by extramedullary haemopoeisis
• NOTE: other myeloproliferative disorders can transform into myelofibrosis

Question 20

Outline the typical presentation of primary myelofibrosis.

Answer 20

• Cytopaenias (anaemia, thrombocytopaenia)
• Thrombosis
• MASSIVE splenomegaly
• Hepatomegaly
• Hypermetabolic state (FLAWS)

Question 21

What might you expect to see in the blood film of a patient with primary myelofibrosis?

Answer 21

• Leucoerythroblastic picture
• Tear drop poikilocytes
• Giant platelets
• Circulating megakaryocytes

Question 22

What is a characteristic feature seen on bone marrow aspirate in primary myelofibrosis?

Answer 22

Dry tap

Question 23

What might you see on histological analysis of a trephine biopsy in primary myelofibrosis?

Answer 23

• Increased reticulin and collagen fibrosis
• Prominent megakaryocyte hyperplasia and clustering
• New bone formation

Question 24

Which mutations would you test for in a patient with primary myelofibrosis?

Answer 24

JAK2 and Calreticulin

NOTE: these are not diagnostic

Question 25

What are some bad prognostic features in primary myelofibrosis?

Answer 25

• Severe anaemia
• Thrombocytopaenia
• Massive splenomegaly

NOTE: median survival is 3-5 years

Question 26

Outline the treatment options for primary myelofibrosis.

Answer 26

• Supportive - RBC and platelet transfusions (usually ineffective becasue of splenomegaly)
• Hydroxycarbamide (may worsen anaemia)
• Ruxolitinib - JAK2 inhibitor
• Allogeneic stem cell transplantation
• Splenectomy - dangerous operation but may provide symptomatic relief

Question 27

What might you expect to see in the FBC of a patient with CML?

Answer 27

• Leucocytosis (MASSIVE)
• Normal or raised Hb and platelets

Question 28

What would you expect to see in abundance in the blood film of a patient with CML?

Answer 28

• Neutrophils
• Basophils
• Myelocytes (NOT blasts)

NOTE: myelocytes are immature myeloid cells that are NOT blasts (analogous to reticulocytes for red blood cells)

Question 29

Briefly describe the natural history of CML before targeted treatment was available.

Answer 29

• 5-6 years stable phase
• 6-12 months accelerated phase
• 3-6 months blasst crisis

Question 30

What is the Philadelphia chromosome?

Answer 30

CML is caused by a translocation between 9;22 producing a derivative chromosome, 22q, which is called the Philadelphia chromosome

Question 31

What are the two genes that make up the fusion gene in the Philadelphia chromosome?

Answer 31

Bcr = breakpoint cluster region

Abl = ableson tyrosine kinase

Question 32

Explain how this fusion gene results in excessive proliferation of myeloid cells.

Answer 32

• Abl is a tyrosine kinase that drives cell proliferation but is rarely expressed unless the cells are receiving a stimulus to proliferation
• Bcr is a housekeeping gene that is constitutively active
• The Bcr-Abl fusion gene means that the tyrosine kinase component is constitutively activated thereby driving cell proliferation in the absence of a stimulus

Question 33

List some diagnostic techniques used to identify the CML and monitor response to treatment.

Answer 33

• FBC and leucocyte count
• Cytogenetics and detection of Philadelphia chromosome (FISH)
• RT-PCR to detect and quantify the number of copies of Bcr-Abl fusion transcript

NOTE: RT-PCR transcript % is the most sensitive

Question 34

What are some issues associated with 1st generation Bcr-Abl tyrosine kinase inhibitors?

Answer 34

• Some people fail to achieve a complete cytogenetic response
• Non-compliance
• Side-effects (fluid retention, pleural effusion)
• Loss of major molecular response (due to resistance mutations)

Question 35

List some examples of Bcr-Abl tyrosine kinase inhibitors.

Answer 35

• 1st generation: imatinib
• 2nd generation: dasatinib, nilotinib
• 3rd generation: bosutinib

Question 36

What are the next steps in treatment if the first-line fails?

Answer 36

• 1st line fails (no complete cytogenetic response at 1 year or initial response is followed by resistance) → switch to 2nd or 3rd generation
• 2nd line fails (inadequate response or disease progresses to accelerated or blast phase) → allogeneic stem cell transplantation