Acute myeloid leukaemia

INVESTIGATIONS

Bone marrow biopsy and aspirate, peripheral blood smear, and immunophenotyping can establish the diagnosis.

Blast cells in ALL are positive for terminal deoxynucleotidyl transferase (TdT) and lack staining for myeloperoxidase; also demonstrate presence of lymphoid markers.

INVESTIGATIONS

Expression of antigens representing both myeloid and lymphoid leukaemia in the leukaemic clone suggests biphenotypic leukaemia.

The presence of the Philadelphia chromosome (BCR::ABL1 fusion gene) supports a diagnosis of biphenotypic leukaemia, but does not exclude Philadelphia chromosome-positive AML.

INVESTIGATIONS

Sustained/persistent eosinophilia (or tissue eosinophilia in a target organ) with elevated serum tryptase.[58]National Comprehensive Cancer Network. NCCN clinical practice guidelines in oncology: myeloid/lymphoid neoplasms with eosinophilia and tyrosine kinase gene fusions​ [internet publication]. https://www.nccn.org/guidelines/category_1

The presence of tyrosine kinase gene fusions (e.g., PDGFRA, PDGFRB, FGFR1, JAK2, ABL1, FLT3).​[58]National Comprehensive Cancer Network. NCCN clinical practice guidelines in oncology: myeloid/lymphoid neoplasms with eosinophilia and tyrosine kinase gene fusions​ [internet publication]. https://www.nccn.org/guidelines/category_1 ​​​​​ 

INVESTIGATIONS

The distinction between high-risk MDS and AML is based on the numbers of blasts present. However, the estimation of blast counts can be difficult and is subjective. The blood film shows dysplasia in >10% of cells of any lineage, and the bone marrow may show ≤19% blasts.

Micromegakaryocytes and acquired Pelger-Huet (spectacle eye nucleus) neutrophils are specific for MDS. Associated chromosomal deletions or unbalanced chromosomal abnormalities, particularly of chromosomes 8, 7, and 5, are common. Complex cytogenetic changes may occur.

The presence of dysplasia may suggest that AML has evolved from MDS.

INVESTIGATIONS

Blood film may be indistinguishable from AML but may have an excess of basophils and eosinophils.

The presence of the Philadelphia chromosome (BCR::ABL1 fusion gene) supports a diagnosis of CML, but does not exclude Philadelphia chromosome-positive AML.

Typically no other karyotypic abnormalities are present.

INVESTIGATIONS

Blood film shows teardrop red blood cells and a leukoerythroblastic film.

Bone marrow biopsy shows reticulin fibrosis.

INVESTIGATIONS

A negative Coombs test suggests aplastic anaemia.

Bone marrow biopsy and aspirate are hypocellular.

Low percentage of blast cells in peripheral blood (<10%). Precursors are morphologically normal.

Patients may have concurrent paroxysmal nocturnal haemoglobinuria clone and evidence of intravascular haemolysis (reticulocytosis, elevated serum lactate dehydrogenase, indirect bilirubin, decreased haptoglobin).

INVESTIGATIONS

Bone marrow biopsy and aspirate will be hypocellular, and no excess of blasts are present.

Peripheral blood smear may be helpful.

Megaloblastic erythropoiesis is seen with methotrexate.

Bone marrow should be reassessed after drug cessation.

INVESTIGATIONS

Bone marrow biopsy and aspirate, and peripheral blood smear are helpful in differentiating diagnosis.

Bone marrow shows no excess of blasts, but does show mature haematopoietic cells. Increased macrophage activity and toxic granulation of myeloid cell series may be present, suggesting infections; Dohle bodies may also be seen in infections.

INVESTIGATIONS

Macrocytic anaemia will be present unless there is an associated iron deficiency.

Peripheral blood smear shows megaloblastic changes.

Serum vitamin B12 levels are low.