63771
Haemopoietic System Malignancies
- Haemopoietic stem cells
- Progenitor cells
- Mature blood cells
- Lymphoid Progentior
- B cells
- Plasma cells
- B cell lineage lymphomas, myeloma, chronic
lymphocytic leukaemia, Hodgkins disease
- Plasma cells
- T cells
- T lineage lymphomas (less common than B)
- T lineage lymphomas (less common than B)
- NK cells
- Pre B acute lymphoblastic leukaemia, T lineage
precursor acute lymphoblastic leukaemias
- B cells
- Myeloid Progenitor
- Erythrocyte
- Megalokarocyte
- Platelets
- Platelets
- Neutrophil
- Eosinophil
- Basophil
- Acute myeloid leukaemia
- Erythrocyte
- Lymphoid Progentior
- Lifespan-months (short)
- Mature blood cells
- Cannot survive without
- Chronic myeloid leukaemia, myelodysplastic
syndromes, acute myeloid leukaemias
- Progenitor cells
- Leukaemia
- 'White blood'
- 2 types
- Acute leukaemia
- Accumulation of blasts (undifferentiated
cells) in bone marrow/blood
- 2 types
- Acute myeloid leukaemia - cells derived from
haematopoietic stem cells/myeloid progenitors
- More common in older
people - peak 80-84
- More common in older
people - peak 80-84
- Acute lymphoblastic leukaemia - cells
derived from lymphoid precursors
- Childhood leukaemia -
most common 5-9 yo
- Childhood leukaemia -
most common 5-9 yo
- Acute myeloid leukaemia - cells derived from
haematopoietic stem cells/myeloid progenitors
- Indices bone marrow failure -
reduced production of blood cells
- Red blood cells - anaemia
- Platelets - spontaneous bleeding - death
- Neutrophils - neutropenic sepsis - death
- Can present with infiltration by
proliferating blasts - less common (usually in blood)
- Other symptoms -
lymphadenopathy, fevers, bone pain
- Red blood cells - anaemia
- Diagnosis by immunophenotyping
- Morphology is not reliable - all look the same
- Morphology is not reliable - all look the same
- Accumulation of blasts (undifferentiated
cells) in bone marrow/blood
- Chronic myeloid leukaemia
- Myeloproliferative disease
- High white blood cell count - cells
differentiate and function normally
- Increased neutrophils and
myelocytes (neutrophil precursor)
- Increased neutrophils and
myelocytes (neutrophil precursor)
- Causes splenomegaly (pain and
satiety), weight loss and fevers
- Deaths are due to transformation
to acute leukaemia (blast crisis)
- WBCs stop differentiating and cannot function
- WBCs stop differentiating and cannot function
- 50% are dead by 4 years
- Philadelphia chromosome is diagnostic
of CML (can occur in acute too)
Annotations:
- See Philadelphia Chromosome section of cancer lecture for more detail
- Karocyte always tested if CML is a possibility
- G-banding - cells in metaphase stained with giemsa
- G-banding - cells in metaphase stained with giemsa
- Bcr/Abl tyrosine kinase causes
- Cell proliferation via JAK/STAT
and MAPK pathway in the nucleus
- Cell proliferation, survival and differentiation
via JAK/STAT and BCL2 family
- Increased motility, decreased
adhesion via Paxillin
- Cell proliferation via JAK/STAT
and MAPK pathway in the nucleus
- Imantinib (Gleevec) blocks Bcr/Abl ATP
site - inhibits tyrosine kinase activity
- Only a few side effects - rash, cramps, oedema, tiredness
- 93% of patients had no blast crisis within 4 years
- Only a few side effects - rash, cramps, oedema, tiredness
- Myeloproliferative disease
- Acute leukaemia
- 'White blood'
- Immunophenotyping
- Antibody with green fluorescent conjugate
binds to specific cell protein (e.g. CD10)
- Different antibody with red fluorescent conjugate
binds to another cell protein (e.g. CD22)
- Cells passed through flow cytometer - flow single file
- Laser shines light onto cells
- Fluorescent proteins emit light of different wavelengths (colours)
- Each colour detected by a different channel
- Results shown on graph
- Results shown on graph
- Each colour detected by a different channel
- Fluorescent proteins emit light of different wavelengths (colours)
- Laser shines light onto cells
- Antibody with green fluorescent conjugate
binds to specific cell protein (e.g. CD10)
- Genetic Testing
- Routine in acute leukaemia diagnosis and management
- Cytogenetics - chromosome structure
- G-banding
- Cells cultured and metaphase spreads made
- Karyotype analysed
- Karyotype analysed
- Cells cultured and metaphase spreads made
- FISH
- Cells don't need to be in metaphase
- Can see the presence of specific loci
using different fluorescent markers
- Cells don't need to be in metaphase
- Cytogenetic abnormalities affect prognosis
- t(12;21) is a good
marker for ALL
- Philadelphia chromosome and t(4;11)
are bad markers - also seen in CML
- Philadelphia chromosome and t(4;11)
are bad markers - also seen in CML
- G-banding
- Point Mutations
- Half of all AML has normal
G-banding/cytogenetic analysis results
- Smaller lesions not detectable by cytogenetics.FISH
- Falini 2005
- 61% of normal karyotype AML has a
mutated nucleophosmin gene
- 61% of normal karyotype AML has a
mutated nucleophosmin gene
- Smaller lesions not detectable by cytogenetics.FISH
- Routine in acute leukaemia diagnosis and management
- Genetic Lesions
- Balanced Translocations
- 8-21 causes AML1-ETO fusion
- AML1 (RUNX1) is a transcription factor on
21, involved in haematopoietic differentiation
- AML1 (RUNX1) is a transcription factor on
21, involved in haematopoietic differentiation
- 9-11 causes MLL-MLLT3 fusion
- MLL is a histone methyltransferase on
chromosome 11, involved in epigenetic regulation
- MLL is a histone methyltransferase on
chromosome 11, involved in epigenetic regulation
- 8-21 causes AML1-ETO fusion
- Mutations
- CEBPA, WT1, RUNX1
all transcription factors
- DNMT3A, TET2, MLL-PTD, ASXL1
all involved in epigenetic regulation
- FLT3, KIT are receptor tyrosine kinases
- CEBPA, WT1, RUNX1
all transcription factors
- Balanced Translocations
- Acute Leukaemia Treatment
- Risk is determined based on cytogenetics and mutations
- Low risk - 4 cycles of intensive chemotherapy
- Multi-drug treatment
- Multi-drug treatment
- Intermediate/High risk - chemotherapy until
remission and then an allogeneic transplant
- Remission = normal bone marrow
and reversal of bone marrow failure
- Remission = normal bone marrow
and reversal of bone marrow failure
- Low risk - 4 cycles of intensive chemotherapy
- No new drugs since 1960/70s
- Daunorubicin (red) and Cytarabine (clear)
- Daunorubicin (red) and Cytarabine (clear)
- AML cells disappear after 2 weeks of constant
RBC and platelet transfusions with antibiotics
- Neutrophil count doesn't increase until much later
- Neutrophil count doesn't increase until much later
- Allogeneic transplant uses graft vs host
reaction to kill remaining cancer cells
- Very unpredictable - can be fatal
- Very unpredictable - can be fatal
- 80% of children can be cured, adults don't do as well
- Risk is determined based on cytogenetics and mutations
Want to create your own Mind Maps for free with GoConqr? Learn more.