Heterogeneous group of hematopoietic neoplasms Uncontrolled proliferation and decreased apoptotic activity with variable degrees of differentiation Composed.

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Presentation transcript:

Heterogeneous group of hematopoietic neoplasms Uncontrolled proliferation and decreased apoptotic activity with variable degrees of differentiation Composed of relatively mature cells Indolent. ( If untreated, the course is in months or years) Occurs mainly in adults Chronic Leukaemias

ErythroblastMegakaryoblast HSC

ChronicAcute LPN(CLL)ALL Lymphoid MPN/MDS (CML) AML Myeloid Acute Biphenotypic Mixed Acute Undifferentiated Non Main Types of Leukemia

44 ALL AML CML CLL

Malignant proliferation of myeloid cells (maturing cells) which are mainly granulocytes, in blood and bone marrow. Occur mainly in adults Slow onset and long course Myeloproliferative Neoplasms

Cytoses Organomegaly (mainly splenomgaly) High uric acid Hypercellular bone marrow Progression to acute leukaemia (mainly AML) MPN features

8 Stem cell MPN. Predominant proliferation of granulocytic cells. Consistently associated with the BCR-ABL1 fusion gene located in the Philadelphia (Ph) chromosome which results from t(9;22). Chronic Myeloid Leukemia (CML)

Activation of signal transduction pathways Tyrosine Kinase Uncontrolled proliferation Pathogenesis of CML

ABLBCR p210 kD Pathogenesis of CML

 Asymptomatic presentation(20-40%):  Routine CBC : marked leukocytosis  Common symptoms : Fatigue,weight loss or night sweating  Abdominal discomfort due to splenomegaly  Splenomegaly (Massive ) Clinical Presentation

LeukaemoidCML Any ageAdultAge High but <100,000HighWBC count Mainly BandsMainly myelocytes and segmentedDifferential ToxicHypogranularMorphology -/++Splenomegaly HighLowNAP score -ve+veBCR/ABL AcuteChronicOnset Main Differential Diagnosis 1- Chronic myelomonocytic leukemia (monocytosis,BCR-ABL –ve). 2-Leukemoid reaction: Leukocytosis due to physiological response to stress or infection

Neutrophil Alkaline Phosphatase (NAP)score : Cytochemical stain that estimate the amount of alkaline phosphatase enzyme in neutrophilis. Low : CML High: Leukemoid

Leukocytosis ( ×10⁹/L) Mainly neutrophils & myelocytes Blasts ≤10%,Basophils≤ 20% Stable course (years) Increasing counts 10-19% blasts (basophils ≥20%) Unstable course (months) ≥20% blasts = Acute Leukemia 80% AML & 20% ALL (coarse: Weeks) Chronic phase Accelerated phase Blastic phase CML Phases

Targeted therapy (tyrosine kinase inhibitors like Imatinib) Excellent response (5y overall survival≥ 90%) If no response ; stem cell transplantation CML Treatment

Group of myeloid neoplasms characterized by: 1-Peripheral cytopenia ( Low HB ± Low WBC & Low PLT ) 2- Dysplasia (abnormal morphology) 3- Ineffective hematopoiesis (hypercellular marrow) 4-Progression to AML (preleukaemic disease) 5-Enhanced apoptosis Myelodysplastic Syndromes MDS

Blood : Pancytopenia with dysplasia BM : Hypercellular with dysplasia Ineffective Hematopoiesis ProliferationApoptosis Myelodysplastic Syndromes MDS Normal Dysplastic

18 MDS

Many subtypes according to: 1-Blast count 2-Degree of dysplasia 3-Genetics Variable genetic abnormalities mainly -5, -7 Treatment : supportive +/- chemotherapy Myelodysplastic Syndromes MDS

Clonal Hematopoietic malignancy characterized by proliferation of both monocytes and neutrophils. MDS/MPN disease: * Features of MDS (dysplasia& enhanced apoptosis) *Features of MPN ( marked proliferation) Philadelphia chromosome must be negative Blast must be less than 20%. Chronic Myelomonocytic Leukemia (CMML )

Aggressive course (survival rate around 2.5 y) Treatment : Chemotherapy ±SCT CMML

MPN MPN/MDS MDS CytosisCytopenia MPN vs. MDS vs. MPN/MDS

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