Y2 Leukaemia

Question 1

What is the site disease in Leukaemia?

Answer 1

Leukaemia is “cancer of the blood”, more specifically

• bone marrow disease (not all patients have abnormal cells in the blood)
• it is cancer in lymphoid/myeloid stem cells

Question 2

What are the different types of cells that can be affected in leukaemia?

Answer 2

1. Pluripotent haematopoietic Stem Cell
   
   • would lead to mixed phenotype leukaemia
   1. Myeloid Stem Cell
      
      1. Myeloid leukaemia
   2. Lymphoid Stem Cell
      
      1. Lmphatic leukaemias
      2. Pre B Lymphocyte
      3. Pro T Lymphocyte

Question 3

Explain and summarise the development of leukaemias

Answer 3

Leukaemias need

• multiple mutations in a single myelod/lympoid stem cell
  
  • leading to a potency of cell for increased proliferation, differentiation, or cell survival
• Leading to expansion of the leukaemic clone

Question 4

Why can’t the concepts of invasion and metastisis not be applied to leukaemias?

Answer 4

Because blood cells (also haematopoietic stem cells) are physiologically found in the body and infiltrate tissues

Question 5

How are “benign” and “malignant” forms of leukaemia determined and named?

Answer 5

The words chronic and acute are used

1. Chronic
   
   • behave in a “benign” manner, the disease goes on for a long time
2. Acute
   
   • behaves “malignant”, untreated the disease is agressive and the patient dies rapidly

Question 6

How are the chronic and acute forms of leukaemias derived from lymphoid precursor cells called?

Answer 6

–Acute lymphoblastic leukaemia (ALL)

–Chronic lymphocytic leukaemia (CLL)

Question 7

How are leukaemias derived from Myeloid cells called?

Answer 7

Acute/Chronic myeloid leukaemias

Question 8

What are the important factors in the development of leukaemia?

Answer 8

Requires a series of mutations (basically just like any other cancer)

Importnatn identified mutations include

• There are normally multiple genes affected, in particular transcription factors so that the transcription of multiple genes is affected and cell behavior profoundly disturbed
  
  • in proto-oncogenes
  • creatin of a novel gene (chiameric/fusion gene)
  • mutation in promoter/enhancer of a structurally normal gene
  • loss of TSG

Question 9

What are certain risk factors to the development of leukaemias?

Answer 9

Some inherited mutations e.g. in

• down syndrome
• defects in DNA repair etc.

Or exposure to

• Irradiation
• Anti-cancer drugs
• Cigarette smoking
• Chemicals—benzene

Question 10

What happens during AML?

Answer 10

, cells continue to proliferate but they no longer mature so there is

• Built up of immautre (myeloblast) cells in the BM and spread into the blood
• Together with a Failure to produce normal cells e.g. neutrophils, monocytes, erythrocytes, platelets

Failure of production of End Cells

Question 11

What are the genetic causes for the production of AML?

Answer 11

• Often Transcription factors involved
  
  • Transcripition of multiple genes affected
• Normal function of proteins are not possible (because they are supressed by an oncogene product)

–> Cell behaviour is profoundly disturbed

Question 12

What are the genetic causes for developement of CML?

Answer 12

mutations usually affect a gene encoding a protein in the signalling pathway between a cell surface receptor and the nucleus

Question 13

What happes during CML?

Answer 13

• cell kinetics and funcitons are not as seriously affected as in AML
• BUT: reduced apoptosis and increase proliferation –> slow progression of leukaemic clones

Increased production of end cells

Question 14

What is the Differnce between acute and chronic LL?

Answer 14

• •Acute lymphoblastic leukaemia (ALL)
  
  • increase in immature cells (lymphoblasts)
  • no maturation into B and T cells
• Chronic lymphoid leukaemias (CML)
  
  • , the leukaemic cells are mature,
  • although abnormal, T cells or B cells

Question 15

What are the general symptoms of leukaemia?

What is the underlying cause?

Answer 15

Normally caused by an accumulation of cells or infiltration of tissues

• bone pain (if acute)
  
  • high metabolic rate and high proliferation
• hepatomegaly and splenomegaly
  
  • extramedullary blood formation (due to no more formation in BM) and increased infiltration of tissues by cells
• lymphadenopathy (if lymphoid),
• thymic enlargement (if T lymphoid),
• skin infiltration
• overall: increased metabolic rate
  
  • weight loss sweating, low grade fever

Question 16

What are general haematological findings that cause symptoms in Leukaemia?

Answer 16

•Crowding out of normal cells leading to

• anaemia,
• neutropenia,
• thrombocytopenia

–> + associated symptoms

In CLL

• loss of function of T+B-lymphocytes: loss or normal immune function
  *

Question 17

When does Acute lymphblastic leukaemia usually occur?

What might protect you from developing ALL?

Answer 17

Main incidence in children

• Protective: early exposure to common antigens
  
  • relates to family size, new towns, socio-economic class, early social interactions, variations between countries

Question 18

What might be causes of ALL in children?

Answer 18

Some (limited) evidence for:

• Irradiation in utero
• In utero exposure to certain chemicals ? Baygon, ? Dipyrone
• ? Epstein–Barr virus infection

•Rarely any ALL results from exposure to a mutagenic drug

Question 19

What are symptoms of ALL?

Answer 19

Resulting from accumulation of abnormal cells (+inflitration of tissues) leading to:

• Bone pain
• Hepatomegaly
• Splenomegaly
• Lymphadenopathy
• Thymic enlargement
• Testicular enlargement

And Resulting from crowding out of normal cells (ANT symptoms)

• Anaemia casuing Fatigue, lethargy, pallor, breathlessness
• Neutropenia: Fever and other features of infection
• Thrombocytopenia: Bruising, petechiae, bleeding

Question 20

What are haematological findings in ALL?

Answer 20

• Leucocytosis with lymphoblasts in the blood
• Anaemia (normocytic, normochromic)
• Neutropenia
• Thrombocytopenia
• Replacement of normal bone marrow cells by lymphoblasts

Question 21

Which investigations would you perform in someone you suspect having an ALL?

Answer 21

• Blood count and film
• Check of liver and renal function and uric acid (because of high DNA turnover)
• Bone marrow aspirate
• Cytogenetic/molecular analysis –> which type of ALL?
• Chest X-ray (thymoid swelling)

Question 22

Explain the importance of immunophenotyping in ALL

Answer 22

It is important to determine the cause of the Leukaemia

• B cell? T cell?
• Done by flourescent analysis of cells (binding to CD factors of cells)

Question 23

Explain the use of cytogenetic and molecular genetic analysis in ALL

Answer 23

Analysisng individual patient to determine prognosis

• E.g. •Hyperdiploidy—good prognosis
• •t(4;11) translocation—poor prognosis

Question 24

Which genetic factors often lead to the development of ALL?

Answer 24

• Formation of a fusion gene (translocation) (9,22 Philadelphia and 12+21) –> production of abnormal intracellular proteins
  
  • can be detected via FISH analysis
• Dysregulation of a proto-oncogene by juxtaposition of it to the promoter of another gene, e.g. a T-cell receptor gene (tranlocations)
• Point mutation in a proto-oncogene

Question 25

Summarise the treatment in ALL

Answer 25

1. Supportive treatment
   
   1. blood/platelet transplants if needed
   2. antibiotics in signs of infection
2. Systemic chemotherapy
3. Intrathecal chemotherapy –> otherwise poorer prognosis+ higher chance of return of disease (often vie LP)

Question 26

What is the prognosis of an ALL with trisomy 4?

Answer 26

-good