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Michael Dickinson, Haematologist Peter MacCallum Cancer Centre Myelodysplasia: background and current treatment approaches in Australia Overview • What is myelodysplasia? How does it affect you? • How doctors think about the disease and the words we use? • What on earth is epigenetics? • Treatments – When, what, how, practicalities…. Azaciditine & lenalidomide (MDS) • Trials Understanding myelodysplasia isn’t easy! Effects of MDS • • • • Low white cell count (neutropenia) Low red cell count (anaemia) Low platelet count (thrombocytopenia) In some patients there is a risk of leukaemia What is myelodysplasia (MDS)? • “clonal disorder of the bone marrow” • MDS is a kind of cancer Myeloproliferative disorders • Also a clonal disorder • Large spleen &/or liver • High white cell count, red cell count, or platelets Clones. Causes ? DIAGNOSIS Basic Diagnostic Evaluation FBE, film Bone marrow aspiration and biopsy Cytogenetics (flow cytometry) Additional tests Vitamin levels (B12, folate, iron and ferritin) EPO (erythropoietin) Other eg causes anaemia Diagnosis • Low counts • The way the precursors look under the microscope • More than the normal amount of blasts. What are “blasts”? Classification of MDS - marrow Percentage of blasts <5% •Normal •Refractory anaemia (RA) •Refractory anaemia with multilineage dysplasia (RCMD) 5-9% •Refractory anaemia with excess blasts 1 (RAEB-1) •CMML-1 10-19% •Refractory anaemia with excess blasts 2 (RAEB-2) •CMML-2 Cytogenetics Prognosis - IPSS Cytogenetics Percent blasts in the marrow Number of cytopenias IPSS score Prognosis – R-IPSS Cytogenetics (more categories) Number of cytopenias with severity scoring R-IPSS (more categories) Percent blasts in the marrow (altered cutoffs) TREATMENT - MDS Managing marrow failure:T ransfusion • Red cells • Platelets • ?white cells For many people people, transfusion is no problem but sometimes there are complications • Inconvenient • Platelet transfusion refractoriness “platelet antibodies” • Red cell transfusion refractoriness “red cell antibodies” • Rate of transmitted disease is very low – ARCBS keeps blood safe. Iron overload • Haemoglobin contains iron • Ferritin > 1000 (20units) • Evidence of iron overload Iron overload Exjade • Iron chelator • Orally available • Generally well tolerated • Some side effects Median Change in Serum Ferritin Levels from Baseline (By Initial Dose Group) Median Change in Serum Ferritin Levels (µg/L) Initial deferasirox dose, mg/kg/day 5–10 (n = 227) 20 (n = 182) 30 (n = 243) 1000 500 0 -500 −1000 Extension Core −1500 0 2 4 6 8 10 12 14 16 18 20 22 24 26 28 30 32 34 36 38 40 42 Time Since Start of Treatment (months) Studies 106–109 With permission from Porter J, et al. ASH 2007. December 8-10, 2007. Poster 968. Other treatments • Erythropoietin in renal failure • Immunosuppression in rare cases New treatments for MDS • • • • Big steps forward Azacitidine (Vidaza) Lenalidomide (for 5q-) (Revlimid) New trials Epigenetics • Things that change the way genes are expressed without changing the DNA code. • Histone modification • DNA methylation Azacitidine (Vidaza) • Epigenetic drug • “low dose chemotherapy” Azacitidine (VIDAZA) • • • • Subcutaneous injection 7 days each month Given as a maintenance therapy PBS funded - >10% blasts, <30% blasts Reduces the risk of progression to leukaemia • Reduces transfusion dependence Better than “best supportive care” and conventional chemotherapy Key issues around azacitidine • Initial cytopenia cycle 1-2 (and sometimes ongoing) • Response at 4 cycles. • 7 consecutive days of therapy • Skin irritation • Azacitidine breaks conventional thinking. • PBS approval Example of patient: 5-azacitidine Lenalidomide (Revlimid) • Tablet - well tolerated. Best evidence 5qdisease • Available in Australia but not funded for myelodysplasia • Expensive • Reduces transfusion requirements but not a treatment for blasts • Side effects include low neutrophils and platelets • Doesn’t work in everyone • In high doses maybe anti-leukaemic Other supportive things • Antibiotics – posaconazole (noxafil) Allotransplantation • Mini-allo transplant • Uncertainty about timing Why MDS studies are challenging • Toxicity of novel agents • Measuring responses • Leukemic transformation is part of the natural history • Drug development is also a business Trials • MDS4 (Aza-rev) Trials • MDS4 (Aza-rev) • Aza-eltrombopag Eltrombopag Eltrombopag plus azacitidine Azacitidine alone Trials • • • • • MDS4 (Aza-rev) Aza-eltrombopag Aza-panobinostat Phase 1 studies International studies – Eltrombopag – Estybon (rigosertib, ON 01910.NA) – cell cycle inhibitor via polo-like kinase inhibition – Tosedostat – aminopeptidase inhibitor – HDAC inhibitor combination studies Conclusions • Myelodyspasia is heterogenous (everybody’s case is different) • Many advances in the last few years • Much progress in supportive care • Victoria is a great place to be!