Introduction to Leukaemia

Question 1

Define Leukemia

Answer 1

Leukaemia = A group of malignant disorders of HSCs, characteristically associated with ↑ WBCs in BM and/or peripheral blood

Question 2

Major classifications of leukaemia

Answer 2

Lymphoid vs Myeloid
Acute (Undiff) vs Chronic (Diff)

Question 3

Haematopoiesis site at gestation
Haematopoiesis site in child/adult

Answer 3

Haematopoiesis site at gestation - liver + spleen
Haematopoiesis site in child/adult - bone marrow

Question 4

What types of progenitor cells are there ?

Answer 4

1. Undifferentiated (multipotent) progenitors - You cannot differentiate between myeloid /lymphoid because they do not show the characteristics of mature cells
2. Totipotent/unipotent progenitors - These are committed progenitor cells = have already committed to what they will become when they generate mature cells.

Question 5

What cells does Leukemia affect ?

Answer 5

Lymphocytes
Neutrophils
Eosinophils
Basophils
Monocytes
Platelets

Question 6

What are formed from haematopoietic stem cells?

What are progenitor cells?

Answer 6

Haematopoietic stem cells differentiate to produce :
-Common myeloid progenitor and -Common lymphoid progenitor

Progenitors:

• Can divide to produce many mature cells (blood cells)
• Cannot divide indefinitely = eventually differentiate and mature

Heterogeneous pool of progenitors

Question 7

HSCs potency =

Undifferentiated Progenitor cells potency =

Committed Progenitor cells potency =

Answer 7

HSCs = multipotent

Undifferentiated Progenitor cells = multipotent

Committed Progenitor cells = unipotent

Question 8

What are hematopoietic stem cells (HSCs) and their features?

Answer 8

HSCs = multipotent = can give rise to cells of every blood lineage

• Self-renew - HSCs can divide to produce more stem cells
• Can divide asymmetrically/symmetrically
• Following asymmetric division, HSC forms more differentiated cells with less potency capacity.
• Asymmetric division maintains pool of stem cells.

Question 9

What type of disease is leukaemia?

How does leukaemia arise?

Answer 9

Leukaemia = a clonal disease - All the malignant cells derive from 1 single mutant stem cell.

First Mutation in a HSC/progenitor = ↑ oncogenic TFs = arrest differentiation + self-renew (cells permanently divide) = pre-leukaemic state HSCs/progenitors. (-First mutation = pre-leukaemia)

-Second mutation = leukaemia (↑ survival + proliferation)

Question 10

Outline the incidence of leukaemia

Answer 10

Leukaemia is most common in: 75yrs+ male

Question 11

Describe the presentation of leukaemia

Answer 11

Presentation varies between types of leukaemia

Typically first presents with symptoms of loss of normal blood cell production :

• Abnormal bruising - due to abnormal platelet production
• Repeating abnormal infection (absence of white blood cells = loss of immune function to fight infection, fever)
• Anaemia (↓ production of RBC, ↓ Hb) = fatigue, SOB, paleness, dizzy

BM usually produces RBCs, WBCs, platelets - Not in leukaemia

Question 12

What causes anaemia in Leukaemia ?

Answer 12

Reduced production of RBC

In the bone marrow, 3 lineages of cells are formed:
WBC, RBC and platelets
But in Leukaemia, no production of these cells.

Fatigue
Loss of Immune power
Fever
Dizziness

Question 13

How can we diagnose Leukaemia ?

Answer 13

1. Peripheral blood blasts tests (PB)
   Checks for presence of blasts (immature cells) and cytopenia
   >30% blasts = suspected acute leukaemia
2. Bone marrow biopsy.
   Extract BM from pelvic bone and compare results with PB
3. Lumbar puncture - Determines if the leukaemia has spread to CSF

Question 14

What are the ways in which we can categorise Leukaemia ?

Answer 14

Molecular and pathophysiological characterisation of leukaemia

• Cytomorphology
• Immunophenotyping
• Next generation sequencing (to identify mutations causing leukaemia)
• Fluorescence in situ (FISH) Hybridisation
• Flow cytometry - detect membrane/intracellular markers

Studying cells to identify the molecular markers that characterise the cells - cell surface markers, cell morphology, identify mutations causing leukaemia etc.

After diagnosing leukaemia

Question 15

What is the cause of Leukamia ?

Answer 15

Unclear exact cause of leukaemia

Polyaetiological disease = Combination of predisposing factors - genetic, environmental, lifestyle

Leukaemia = Not usually hereditary disease.
Usually caused by somatic genetic alterations = not present in gametes.

Some rare genetic diseases predispose to leukaemia :
Fanconi’s anaemia, Down syndrome

bc involve genes that are involved in leukaemia = trigger leukaemia as a secondary disease

Question 16

What are the genetic risk factors of developing Leukaemia ?

Answer 16

Gene mutations - activate oncogenes/inactivate tumour suppressors :
-Involving genes common to other malignancies (TP53-Li-Fraumeni syndrome, NF1-Neurofibromatosis = develop leukaemia + other associated disease) or specific to leukaemia

Chromosome aberrations:

• Translocations (BCR-ABL in CML) - 95% of chronic myeloid leukaemia
• Numerical disorders (Down Syndrome trisomy 21) - secondary leukaemia associated w primary disease

Inherited immune system problems:

• Ataxia telangiectasia
• Wiskott-Aldrich syndrome

Question 17

What are some environmental risk factors of developing leukaemia ?

Answer 17

Radiation exposure :

• Acute radiation accidents
• Atomic bomb survivors

Exposure to chemicals and chemotherapy:

• Cancer chemotherapy with alkylating agents
• Industrial exposure to benzene

Immune system suppression:
-Organ transplant

Question 18

What are some lifestyle-related risk factors ?

Answer 18

Adult cancers :

• Smoking
• Alcohol
• Excessive sun exposure
• Overweight

Question 19

What are some possible childhood leukaemia causes ?

Answer 19

• Exposure to electromagnetic fields
• Nuclear power stations
• Infections during early life
• Parents smoking history
• Foetal exposure to hormones
• Mother’s age when child is born

Question 20

What is the classification of Leukaemia ?

Answer 20

There are 4 types of Leukaemia:

• Acute Lymphoid/Lymphoblastic leukaemia
• Chronic Lymphocytic leukaemia
• Acute Myeloid/Myeloblastic leukaemia
• Chronic Myeloid/Granulocytic leukaemia

depending on affected cell lineage + onset+cause of disease

Question 21

Outline Acute Leukaemia

Answer 21

Acute = Rapid onset, short but severe course

• Undifferentiated leukaemia - affects undiff. cells
• Characterised by uncontrolled clonal and accumulation↑ of immature white blood cells (-blast)

Blasts = immature cells - Myeloblast/Lymphoblast

Blood film: ↑ blast cells

slide 26

Question 22

Outline Chronic Leukaemia

Answer 22

Chronic disease = persists over a long time

Chronic leukaemia:

• Differentiated leukaemia - affects differentiated cells (unipotent)
• Characterised by uncontrolled clonal and accumulation↑ of mature white blood cells ( -cyte )

Cytes = mature cells, cells which have differentiated

slide 28

Question 23

Why is it difficult to differentiate between lymphoblast and myeloblast?

Answer 23

• Bc the blast cells are very immature

Question 24

What are the main differences b/w Acute and Chronic?

Age, Onset, Duration, WBC count

Answer 24

Age:

• Acute - Children
• Chronic - Middle aged/Elderly

Onset:

• Acute - Sudden
• Chronic - Insidious

Duration:

• Acute - Weeks/Months
• Chronic - Years

WBC counts:
Acute - Variable
Chronic - High

Question 25

How is acute leukaemia characterised ?

Answer 25

Characterized by a large number of lymphoblasts (ALL)/myeloid blasts (AML) in bone marrow

=Blood - “undifferentiated leukaemia”.

High number of blasts

Question 26

What causes an increase in blast cells in Acute Leukaemia?

Answer 26

Normally the process is:
Cell proliferation → Blast cell pool → Mature cells → Cell death (Apoptosis /Necrosis )

In acute leukaemia:
Cell proliferation → Blast cell pool → (Maturation arrest)
Some cells die before maturing.

Cell proliferation/Cell death imbalance = ↑ blast cells

slide 35

Question 27

What are the typical symptoms of acute leukaemia ?

Answer 27

Typical symptoms of acute leukaemia are due to bone marrow suppression:

Thrombocytopenia: purpura (bruising), epistaxia (nose bleed), bleeding from gums

Neutropenia: Recurrent infections, fever

Anaemia: Fatigue, weakness, tiredness, shortness of breath

Might take a bone marrow biopsy to confirm

Question 28

Describe Acute Lymphoblastic Leukaemia presentation within the population

Prevalence, Origin, Classification, Treatment+Outcome, Remission stats

Answer 28

Prevalence: Childhood

Origin: Cancer of immature lymphoblasts (produce T-cell+B-cell)

Classification: B-cell and T-cell leukaemia

Treatment: Chemotherapy - Long term side effects are rare

Outcome: 5 year event-free survival.

1/10 patients relapse
Remission in 50% after chemotherapy treatment

Adult ALL - poorer prognosis bc disease presents different cell of origin and different oncogene mutations.

Question 29

Describe Acute Myeloblastic Leukaemia and its presentation within the population

Prevalence, Origin, Classification, Treatment+Outcome, Symptoms

Answer 29

Abnormal production of WBCs - neutrophils, eosinophils, monocytes, basophils

Prevalence: 70 children aged under 16 diagnosed every year = v rare

Origin: Cancer of immature myeloid WBC - myeloblasts

Classification: Based on FAB system (M0-M7)

Treatment: Chemotherapy , monoclonal antibodies (immunotherapy), allogenic bone marrow transplant.

Outcome - 5 year event-free survival (50-60%)

Symptoms: More bleeding in AML

Question 30

How to distinguish the difference b/w ALL/AML?

Answer 30

Perform cytomorphological studies to identify the type of blast observed in bone marrow biopsy/blood film

ALL/AML = diff. onset but similar symptoms

Question 31

Chronic leukaemia is characterised by ………..

Answer 31

↑ number of differentiated cells = differentiated leukaemia

Mature cells (WBCs)
Affects cells with lower potency

As haematopoiesis process continues and blood cells mature and differentiate, potency reduces (slide10)

Question 32

Outline Chronic Lymphocytic Leukaemia

Prevalence, Origin, Symptoms, Treatment, Outcome

Answer 32

Prevalence: 3800 new cases every year. Average age = 70

Origin: ↑ numbers of mature(clonal) lymphocytes in bone marrow + peripheral blood

Symptoms: Recurrent infections, Neutropenia , suppresion of normal lymphocyte function, anaemia, thrombocytopenia, lymph node enlargement, hepatosplenomegaly (enlargement of liver + spleen)

Treatment : Regular chemotherapy to ↓ numbers of mature cells

Outcome: 5 year event-free survival of 83%

Question 33

Outline Chronic Myeloid/Granulocytic leukaemia

Prevalence, Cell characteristic, Symptoms, Diagnosis, Treatment, Outcome

Answer 33

Prevalence: 742 new cases/yr diagnosed in UK. Late onset (85/90yo)

Cell characteristic: ↑ numbers of mature myeloid WBC

Symptoms: Often asymptomatic and discovered through routine blood tests

Diagnosis: high white cell count (neutrophilia) in blood and bone marrow, presence of Philadelphia chromosome

Treatment: targeted therapy - Imatinib

Outcome: 5-year event-free survival is 90%. If progresses, then allogeneic BM transplant

Question 34

What is the BCR-ABL oncogene ?

Answer 34

BCR-ABL oncogene = oncogene found through translocation within a small chromosome called Philadelphia chromosome. In 95% CML. Balanced translocation b/w chr9/chr22. slide 45 + notes

BCR - Encodes a protein that needs to be continuously active. Has a strong, active promoter which promotes permanent transcription of BCR gene. Cell needs continuous BCR activity.

ABL - Encodes a protein tyrosine kinase whose activity is tightly regulated (auto-inhibition). Proto-oncogene

BCR-ABL protein has constitutive (unregulated) protein kinase activity as the ABL is now under regulation of the BCR promoter.

slides45/ 46

Question 35

Outline the consequences of unregulated tyrosine kinase activity due to BCR-ABL

Answer 35

• Proliferation of progenitor cells in the absence of growth factors
• Decreased apoptosis
• Decreased adhesion of cells to bone marrow stroma

= together trigger leukaemia

Question 36

What is detected in 95% of CML?

Answer 36

Philadelphia Chromosome - chr fusion

BCR-ABL oncogene

Question 37

What are the applications of the BCR-ABL oncogene ?

Answer 37

95% of cases of CML have a detectable Philadelphia chromosome

Detection of minimal residual disease

Therapy: Drugs that specifically inhibit BCR-ABL e.g. Imatinib
Cases negative for BCR-ABL will require different therapy

Question 38

What is Imatinib ?

(REVISIT)

Answer 38

Imatinib = A small molecule inhibitor that targets specifically ABL-CML treatment

Used to treat CML containing Philadelphia chr. 5% require diff. therapy

Inhibits continuously active TyrKinase activity of fusion protein resulting from translocation.

ABL gene Tyr kinase Requires ATP to work to phosphorylate substrate therefore fusion protein requires ATP to activate.

Imatinib competes w ATP to bind to pocket = ATP cannot bind = fusion protein cannot phosphorylate substrates (tyrosine aa’s of substrate) = oncoprotein cannot activate downstream pathways = treats CML

Remission induced in more patients with greater durability and fewer side effects

Some patients become drug resistant

Abl gene is a tyrosine kinase and contributes ATP.
Competes with ATP therefore the fusion protein wont be able to phosphorylate the substrates.

Question 39

Philadelphia chromosome translocation gives rise to …………………………..

Answer 39

a novel oncogene - BCR-ABL

Question 40

3 stem cell types (potency)

Answer 40

• Totipotent - form following fertilisation, zygote, can diff into all body cells
• Pluripotent - embryo, form all cell types but less versatile than totipotent SCs
• Multipotent - diff into cell lineages: haematopoietic SCs, mesenchymal SCs, neural SCs

Question 41

Main Properties of Stem Cells

Answer 41

• Self-renewal = production of more stem cells
• Proliferation
• Differentiation

Question 42

Haematopoiesis starts with ……..

Answer 42

Haematopoietic CD34+ stem cell = multipotent stem cell.

34 = number of transmembrane phosphoglycoproteins = important marker for HSCs

Question 43

Which pathway is important in haematological cancers?

Answer 43

JAK pathway

Question 44

All blood cells divide into 3 different lineages

Answer 44

Erythrocytes = oxygen-carrying cells, released into blood

Lymphoid lineage = T-lymphocytes, B-lymphocytes, Natural Killer cells. Lymphocytes = derived from common lymphoid progenitors. Adaptive immune system.

Myeloid Lineage = Granulocytes (BEN), Megakaryocytes, Macrophages. Derived from common myeloid progenitors. Innate immune system, blood clotting

Question 45

Progenitor cells can be of 2 diff. types:

Answer 45

• Undifferentiated Progenitor Cells = Multipotent. Not mature cells. Give rise to 2 diff. groups of blood cells (lineages). Common Myeloid Progenitor, Common Lymphoid Progenitor
• Committed Progenitor Cells = Unipotent. Already committed to what they will become when they generate mature cells. Only give rise to 1 type of blood cell.

see slide 9

Question 46

Patients undergoing chemotherapy due to ALL are …………..

Answer 46

highly immunocompromised due to the leukaemia + chemotherapy treatment

= require antibiotics for fever (↑ temp)