Acute Leukemia Cases - Nikcevich Flashcards

1
Q

What is the #1 prognostic feature in leukemia that drives the treatment and prognosis?

A

Cytogenetics

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2
Q

What cytogenetic abnormality has an unfavorable risk in acute leukemia and is associated with previous chemotherapy treatment?

A

11q23

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3
Q

What is the difference between the FAB and WHO classification of acute leukemia?

A
  • FAB: > 30% BM myeloblasts, old, not used much anymore
    • M0 (undifferentiated myeloid)
    • M1 (acute myeloid without maturation)
    • M2 (acute myeloid with maturation)
    • M3 (acute promyelocytic leukemia)
    • M4 (acute myelomonocytic leukemia)
    • M5 (acute monocytic leukemia)
    • M6 (acute erythroleukemia)
    • M7 (acute megakaryocytic leukemia)
  • WHO: >20% BM myeloblasts, new, used more
    • AML with recurrent cytogenetic abnormalities – t(8;21), t(15;17), t(inv16), 11q23
    • AML with multilineage dysplasia
    • AML and MDS, therapy-related
    • AML not otherwise categorized – similar to FAB list
    • Acute biphenotypic leukemia
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4
Q

When is extramedullary disease present?

A
  • Cell maturation outside of bone marrow
  • Most common in monocytic leukemias
    • hypertrophic gums
  • can occur in skin, CNS, orbits, bone, lung, kidney, spleen, liver, ovaries
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5
Q

What is consolidation therapy?

A
  • Treatment after remission
  • killing any remaining cancer cells
    • “mop up” with more chemotherapy
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6
Q

What is allogeneic stem cell transplantation?

A
  • treatment for first or second relapse
  • transplant stem cells from another person
    • donor sources include siblings, children, parents, umbilical cord blood, or matched unrelated donor
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7
Q

When is transplant preferred over consolidation chemotherapy?

A
  • Poor risk cytogenetics
  • Intermediate-risk cytogenetics with matched sibling donor
  • Extramedullary disease (chloroma)
  • 1st or 2nd relapse
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8
Q

What cytogenetics are common with Acute promyelocytic leukemia (M3)?

A
  • Most with t(15;17)
    • creates fusion gene, PML/RAR-alpha
  • Poor risk disease with t(11;17)
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9
Q

If a patient is diagnosed with Acute promyelocytic leukemia (M3) and DIC, what is the goal for treatment?

A
  • Don’t let the sun set on M3!
  • Start ATRA (all-trans retinoic acid) in <6 hours!
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10
Q

What is the common presentation of DIC in the setting of Acute promyelocytic leukemia (M3)?

A
  • Coagulopathy
  • Depressed fibrinogen
  • Thrombocytopenia
  • Fatal hemorrhage
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11
Q

What could cause fatigue, headache, and blurred vision in a patient with AML-M4? Tx?

A
  • Hyperleukocytosis
    • Hyperviscosity
    • sludging in vasculature with ischemia and/or infarct
  • Tx: leukophoresis to reduce WBC to <100K
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12
Q

What should you do if you see a patient for fatigue and fevers that turns out to have a low hemoglobin, normal platelet count, and normal WBC with automated differential reporting monocytosis?

A
  • When see monocytosis on differential → don’t be fooled
    • Automated differential reports monocytosis BUT automatic cell counters can confuse blast cells and monocytes
  • So… look under microscope – bone marrow biopsy shows M4 AML leukemia
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13
Q

What new treatment paradigms will we see for Acute Myelogenous Leukemia in the future?

A
  • Targeted therapies
  • Flt-3 receptor tyrosine kinase inhibitors
    • Quizartinib
    • Effective (47% response rate) in relapsed AML
    • May be effective “bridge to transplant” strategy
  • CBF (core binding factor)
    • Dasatinib
    • C-kit overexpression in CBF + AML
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