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Thomas Froehlich, M.D.
 Classic Myeloproliferative neoplasms (MPN) :
include Polycythemia vera, Chronic Myelogenous
Leukemia, Essential Thrombocythemia, Primary
Myelofibrosis, Chronic Neutrophilic Leukemia,
Chronic Eosinophilic Leukemia and Mast Cell
Disease
 Atypical MPNs include Chronic Myelomonocytic
Leukemia, Juvenile Myelomonocytic Leukemia,
Atypical CML and unclassifiable MDS (MDS/MPN)
 Polycythemia vera – can elevate all
hematologic cell lines
 Chronic myelogenous leukemia – usually
affects granulocytes and platelets
 Essential thrombocythemia – usually affects
platelets
 Primary myelofibrosis
 Chronic Neutrophilic Leukemia
 Chronic Eosinophilic Leukemia
 Mast Cell Disease
 Abnormal driver of cellular proliferation in
involved cell lines
 Loss of apoptosis in those lines
 Increased circulation of cells or cellular
elements
 Signs and symptoms related to cells that are
abnormally increased
 All can convert to acute leukemia
gl J Med 2013D;368:161-170
O'Shea JJ et al. N Engl J Med O'Shea JJ et al. N Engl J Med
2013;368:161-170 2013;368:161-170.
O’Shea JJ et al. NEJM 2013;368:161-170
 Several studies have demonstrated familial
clustering for PV, ET and PMF with evidence
of familial involvement. One study of 458
apparent “sporadic” cases showed that 8.7,
6.0 and 8.2% of patients had affected
relatives
 Evidence of monoclonality is more
complicated. Some patients with ET appear to
have polyclonal hematopoeisis, even with the
JAK 2 mutation, while some normals have
been demonstrated to have monoclonal
hematopoeisis
Symptoms Signs
 Fatigue
 Malaise
 Early satiety
 Weight loss
 Fever
 Abdominal pain
 Bone pain
 Pruritis
 Splenomegaly
 Abnormal blood counts
 Abnormal peripheral
blood smears
 Hyperuricemia and
gout
 Thrombosis or
bleeding
Proposed revised WHO criteria for polycythemia vera
 Proposed criteria for PV:
 Major criteria:Hemoglobin >18.5 g/dL in men, 16.5 g/dL in
women or other evidence of increased red cell volume*Presence of
JAK2 617V>F or other functionally similar mutation such as JAK2
exon 12 mutation
 Minor criteria:Bone marrow biopsy showing hypercellularity for
age with trilineage growth (panmyelosis) with prominent
erythroid, granulocytic, and megakaryocytic proliferation. Serum
erythropoietin level below the reference range for normal.
Endogenous erythroid colony formation in vitro.
 Diagnosis requires the presence of both major criteria and 1 minor
criterion or the presence of the first major criterion together with 2
minor criteria.
 * Hemoglobin or hematocrit greater than 99th percentile of method-specific
reference range for age, sex, altitude of residence or hemoglobin greater than 17
g/dL in men, 15 g/dL in women if associated with a documented and sustained
increase of at least 2 g/dL from an individual's baseline value that can not be
attributed to correction of iron deficiency, or elevated red cell mass greater than 25
percent above mean normal predicted value.
 Increased RBC count and Hgb levels (except
when iron deficient)
 Elevated RBC mass
 Panmyelosis in the bone marrow
 Low EPO level
 Positive JAK 2 mutation
 May also have increased platelets and
granulocytes
 Phlebotomy
 Anticoagulation
 Chemotherapy – antimetabolites-
hydroxyurea, alkylating agent-
chlorambucil (no longer used)
 P 32 (also no longer used)
 JAK inhibitors – ruxolotinib
 Erythromelalgia
 Thrombotic events
 Iron deficiency
 Transformation:
◦Myelofibrosis
◦Acute leukemia
 35 y/o previously healthy man
 9 month history of tachycardia and dyspnea on
exertion
 Dec. 2011, dyspnea becomes more severe
 Hospitalized in Miami when found to have
evidence of acute and chronic P.E.s
 Evidence of pulmonary hypertension and a
possible clot in RV outflow tract
 CBC: WBC 13,000 with increased granulocytes,
Hgb 16 gms and platelets 550,000, positive for
JAK 2 mutation
 Diagnostic criteria of the PVSG — The first large-scale attempt to
diagnose ET in a prospective manner was taken by the Polycythemia
Vera Study Group (PVSG). In order to qualify for this diagnosis, the
patient had to fulfill all of the following criteria:
 Platelet count >600,000/microL (>1,000,000/microL for entering
therapeutic protocols)
 Megakaryocytic hyperplasia on bone marrow aspiration and biopsy.
 Absence of the Philadelphia chromosome
 Absence of infection, inflammation, and other causes for reactive
thrombocytosis
 Normal red blood cell (RBC) mass or a hemoglobin concentration <13
g/dL
 Presence of stainable iron in a bone marrow aspiration or ≤1 g/dL
increase in hemoglobin concentration after a one month trial of oral
iron therapy.
 Patients were also excluded if there was collagen fibrosis involving
more than one-third of the cross-sectional area of the bone marrow
biopsy, or if there were lesser degrees of collagen fibrosis in the
presence of splenomegaly and a leukoerythroblastic blood picture.
These latter patients had a presumptive diagnosis of the cellular phase
of PMF.
 2.5 new cases per 100,000/year
 M:F = 1:2
 In U.S., approx. 6000 new cases/year
 Median age at onset = 60 years
 At least half are asymptomatic at diagnosis
 JAK 2 mutation positive in only 40-50% of
cases
 Other reported mutations: CALR in 15-25%
and MPL in up to 4%
Major causes of reactive thrombocytosis
 Nonmalignant hematologic conditions: Acute blood
loss, Acute hemolytic anemia, Iron deficiency
anemia, Treatment of vitamin B12 deficiency,
Rebound effect after treatment of ITP, Rebound
effect after ethanol-induced thrombocytopenia.
 Malignant conditions: Metastatic cancer,
Lymphoma, Rebound effect following use of
myelosuppressive agents.
 Acute and chronic inflammatory conditions:
Rheumatologic disorders, vasculitides,
Inflammatory bowel disease, Celiac disease,
Functional and surgical asplenia, POEMS syndrome
(osteosclerotic myeloma)
 Tissue damage: Thermal burns, Myocardial
infarction, Severe trauma, Acute pancreatitis,
Post-surgical period, especially post-
splenectomy, Coronary artery bypass
procedures.
 Infections: Chronic infections, Tuberculosis.
 Exercise
 Allergic reactions
 Chronic renal disease: Renal failure,
Nephrotic syndrome.
 Reaction to medications: Vincristine,
Epinephrine, Interleukin-1B, All-trans
retinoic acid
 Vasomotor symptoms: Headache,
Lightheadedness, Syncope, Atypical chest pain
Acral paresthesia, Livedo reticularis
 Erythromelalgia - burning pain of the hands or
feet associated with erythema and warmth.
 Transient visual disturbances (eg, amaurosis
fugax, scintillating scotomata, ophthalmic
migraine
 Thrombosis – up to 18% at presentation
 Hemorrhage – up to 26% at presentation
 Antiplatelet agents – less than
325 mg. aspirin/day
 Hydroxyurea
 Anagrelide
 Radioactive phosphorus (no
longer used)
Proposed revised WHO criteria for primary myelofibrosis
Major criteria:
 Presence of megakaryocyte proliferation and atypia,
usually accompanied by either reticulin and/or collagen
fibrosis, or, in the absence of significant reticulin fibrosis,
the megakaryocyte changes must be accompanied by an
increased bone marrow cellularity characterized by
granulocytic proliferation and often decreased
erythropoiesis (ie, prefibrotic cellular-phase disease),
 Not meeting WHO criteria for PV, CML, MDS, or other
myeloid neoplasm.
 Demonstration of JAK2 617V>F or other clonal marker
(eg, MPL 515W>L/K), or in the absence of a clonal
marker, no evidence of bone marrow fibrosis due to
underlying inflammatory or other neoplastic diseases
Proposed revised WHO criteria for primary
myelofibrosis:
Minor criteria:
 Leukoerythroblastosis
 Increase in serum lactate dehydrogenase level
 Anemia
 Palpable splenomegaly
Diagnosis requires meeting all 3 major criteria and 2 minor
criteria.
 Based on risk profile – high risk: Hgb < 10,
constitutional symptoms
 Allogeneic bone marrow or stem cell
transplant
 Androgens, steroids or Erythropoietin
 Transfusion
 Drugs: Hydroxyurea, Interferon, Anagrelide,
Danazol, Thalidomide, Lenalidomide
 Splenectomy – very risky
 Radiation – more effective for
extramedullary hematopoiesis
 JAK 2 inhibition- Ruxolitinib (Jakafi ) a
specific JAK-STAT pathway inhibitor
CRhange in SpRleen Volume.
Verstovsek S et al. N Engl J Med 2012;366:799-
807.
Verstovsek S et al. NEJM 2012;366:799-807.
Change in Spleen Volume
Change inChange in Symptom Scores Symptom Scores.
Verstovsek S et al. N Engl J Med
2012;366:799-807.
Verstovsek S et al. NEJM 2012;366:799-807.
 Most common MPD, 2nd most common
leukemia in adults, 15-20% of cases
 Incidence is 1-2 cases/100,000/year
 Median age at diagnosis 50-60 years
 3 distinct phases:
◦ Chronic, stable
◦ Accelerated
◦ Blast crisis
 Elevated granulocyte count,
mostly mature but with some left
shift
 Increased basophils
 Splenomegaly
 Increased platelets
 Single genetic change
MD Anderson*
 PB blasts>15%PB blasts
+ pro>30 %
 PB baso>20%
 Platelets <100,000/µL
not related to tx
 Cytogenetic evolution
WHO
 PB or BM blasts 10-19%
PB basophils>20%
 Platelets <100,000/µL,
unrelated to tx
 Cytogenetic evolution
 Platelets >1,000,000/µL
unresponsive to therapy
 Progressive
splenomegaly and
increasing WBC
unresponsive to therapy
 ≥20 percent peripheral blood or bone
marrow blasts. (70% myeloid, 20%
lymphoid, undifferentiated)
 Large foci or clusters of blasts on the
bone marrow biopsy.
 Presence of extramedullary blastic
infiltrates (eg, myeloid sarcoma also
known as granulocytic sarcoma or
chloroma).
 Hydroxyurea
 TKI’s: Imatinib, dasatinib, nilitonib,
ponatinib
 Interferon
 Allogeneic stem cell transplant
 Radiation
 Splenectomy
Myeloproliferative disorders
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Myeloproliferative disorders

  • 2.
  • 3.  Classic Myeloproliferative neoplasms (MPN) : include Polycythemia vera, Chronic Myelogenous Leukemia, Essential Thrombocythemia, Primary Myelofibrosis, Chronic Neutrophilic Leukemia, Chronic Eosinophilic Leukemia and Mast Cell Disease  Atypical MPNs include Chronic Myelomonocytic Leukemia, Juvenile Myelomonocytic Leukemia, Atypical CML and unclassifiable MDS (MDS/MPN)
  • 4.  Polycythemia vera – can elevate all hematologic cell lines  Chronic myelogenous leukemia – usually affects granulocytes and platelets  Essential thrombocythemia – usually affects platelets  Primary myelofibrosis  Chronic Neutrophilic Leukemia  Chronic Eosinophilic Leukemia  Mast Cell Disease
  • 5.  Abnormal driver of cellular proliferation in involved cell lines  Loss of apoptosis in those lines  Increased circulation of cells or cellular elements  Signs and symptoms related to cells that are abnormally increased  All can convert to acute leukemia
  • 6. gl J Med 2013D;368:161-170 O'Shea JJ et al. N Engl J Med O'Shea JJ et al. N Engl J Med 2013;368:161-170 2013;368:161-170. O’Shea JJ et al. NEJM 2013;368:161-170
  • 7.  Several studies have demonstrated familial clustering for PV, ET and PMF with evidence of familial involvement. One study of 458 apparent “sporadic” cases showed that 8.7, 6.0 and 8.2% of patients had affected relatives  Evidence of monoclonality is more complicated. Some patients with ET appear to have polyclonal hematopoeisis, even with the JAK 2 mutation, while some normals have been demonstrated to have monoclonal hematopoeisis
  • 8. Symptoms Signs  Fatigue  Malaise  Early satiety  Weight loss  Fever  Abdominal pain  Bone pain  Pruritis  Splenomegaly  Abnormal blood counts  Abnormal peripheral blood smears  Hyperuricemia and gout  Thrombosis or bleeding
  • 9. Proposed revised WHO criteria for polycythemia vera  Proposed criteria for PV:  Major criteria:Hemoglobin >18.5 g/dL in men, 16.5 g/dL in women or other evidence of increased red cell volume*Presence of JAK2 617V>F or other functionally similar mutation such as JAK2 exon 12 mutation  Minor criteria:Bone marrow biopsy showing hypercellularity for age with trilineage growth (panmyelosis) with prominent erythroid, granulocytic, and megakaryocytic proliferation. Serum erythropoietin level below the reference range for normal. Endogenous erythroid colony formation in vitro.  Diagnosis requires the presence of both major criteria and 1 minor criterion or the presence of the first major criterion together with 2 minor criteria.  * Hemoglobin or hematocrit greater than 99th percentile of method-specific reference range for age, sex, altitude of residence or hemoglobin greater than 17 g/dL in men, 15 g/dL in women if associated with a documented and sustained increase of at least 2 g/dL from an individual's baseline value that can not be attributed to correction of iron deficiency, or elevated red cell mass greater than 25 percent above mean normal predicted value.
  • 10.  Increased RBC count and Hgb levels (except when iron deficient)  Elevated RBC mass  Panmyelosis in the bone marrow  Low EPO level  Positive JAK 2 mutation  May also have increased platelets and granulocytes
  • 11.  Phlebotomy  Anticoagulation  Chemotherapy – antimetabolites- hydroxyurea, alkylating agent- chlorambucil (no longer used)  P 32 (also no longer used)  JAK inhibitors – ruxolotinib
  • 12.  Erythromelalgia  Thrombotic events  Iron deficiency  Transformation: ◦Myelofibrosis ◦Acute leukemia
  • 13.
  • 14.
  • 15.
  • 16.  35 y/o previously healthy man  9 month history of tachycardia and dyspnea on exertion  Dec. 2011, dyspnea becomes more severe  Hospitalized in Miami when found to have evidence of acute and chronic P.E.s  Evidence of pulmonary hypertension and a possible clot in RV outflow tract  CBC: WBC 13,000 with increased granulocytes, Hgb 16 gms and platelets 550,000, positive for JAK 2 mutation
  • 17.  Diagnostic criteria of the PVSG — The first large-scale attempt to diagnose ET in a prospective manner was taken by the Polycythemia Vera Study Group (PVSG). In order to qualify for this diagnosis, the patient had to fulfill all of the following criteria:  Platelet count >600,000/microL (>1,000,000/microL for entering therapeutic protocols)  Megakaryocytic hyperplasia on bone marrow aspiration and biopsy.  Absence of the Philadelphia chromosome  Absence of infection, inflammation, and other causes for reactive thrombocytosis  Normal red blood cell (RBC) mass or a hemoglobin concentration <13 g/dL  Presence of stainable iron in a bone marrow aspiration or ≤1 g/dL increase in hemoglobin concentration after a one month trial of oral iron therapy.  Patients were also excluded if there was collagen fibrosis involving more than one-third of the cross-sectional area of the bone marrow biopsy, or if there were lesser degrees of collagen fibrosis in the presence of splenomegaly and a leukoerythroblastic blood picture. These latter patients had a presumptive diagnosis of the cellular phase of PMF.
  • 18.
  • 19.
  • 20.  2.5 new cases per 100,000/year  M:F = 1:2  In U.S., approx. 6000 new cases/year  Median age at onset = 60 years  At least half are asymptomatic at diagnosis  JAK 2 mutation positive in only 40-50% of cases  Other reported mutations: CALR in 15-25% and MPL in up to 4%
  • 21. Major causes of reactive thrombocytosis  Nonmalignant hematologic conditions: Acute blood loss, Acute hemolytic anemia, Iron deficiency anemia, Treatment of vitamin B12 deficiency, Rebound effect after treatment of ITP, Rebound effect after ethanol-induced thrombocytopenia.  Malignant conditions: Metastatic cancer, Lymphoma, Rebound effect following use of myelosuppressive agents.  Acute and chronic inflammatory conditions: Rheumatologic disorders, vasculitides, Inflammatory bowel disease, Celiac disease, Functional and surgical asplenia, POEMS syndrome (osteosclerotic myeloma)
  • 22.  Tissue damage: Thermal burns, Myocardial infarction, Severe trauma, Acute pancreatitis, Post-surgical period, especially post- splenectomy, Coronary artery bypass procedures.  Infections: Chronic infections, Tuberculosis.  Exercise  Allergic reactions  Chronic renal disease: Renal failure, Nephrotic syndrome.  Reaction to medications: Vincristine, Epinephrine, Interleukin-1B, All-trans retinoic acid
  • 23.  Vasomotor symptoms: Headache, Lightheadedness, Syncope, Atypical chest pain Acral paresthesia, Livedo reticularis  Erythromelalgia - burning pain of the hands or feet associated with erythema and warmth.  Transient visual disturbances (eg, amaurosis fugax, scintillating scotomata, ophthalmic migraine  Thrombosis – up to 18% at presentation  Hemorrhage – up to 26% at presentation
  • 24.  Antiplatelet agents – less than 325 mg. aspirin/day  Hydroxyurea  Anagrelide  Radioactive phosphorus (no longer used)
  • 25.
  • 26. Proposed revised WHO criteria for primary myelofibrosis Major criteria:  Presence of megakaryocyte proliferation and atypia, usually accompanied by either reticulin and/or collagen fibrosis, or, in the absence of significant reticulin fibrosis, the megakaryocyte changes must be accompanied by an increased bone marrow cellularity characterized by granulocytic proliferation and often decreased erythropoiesis (ie, prefibrotic cellular-phase disease),  Not meeting WHO criteria for PV, CML, MDS, or other myeloid neoplasm.  Demonstration of JAK2 617V>F or other clonal marker (eg, MPL 515W>L/K), or in the absence of a clonal marker, no evidence of bone marrow fibrosis due to underlying inflammatory or other neoplastic diseases
  • 27. Proposed revised WHO criteria for primary myelofibrosis: Minor criteria:  Leukoerythroblastosis  Increase in serum lactate dehydrogenase level  Anemia  Palpable splenomegaly Diagnosis requires meeting all 3 major criteria and 2 minor criteria.
  • 28.
  • 29.
  • 30.
  • 31.
  • 32.
  • 33.  Based on risk profile – high risk: Hgb < 10, constitutional symptoms  Allogeneic bone marrow or stem cell transplant  Androgens, steroids or Erythropoietin  Transfusion  Drugs: Hydroxyurea, Interferon, Anagrelide, Danazol, Thalidomide, Lenalidomide  Splenectomy – very risky  Radiation – more effective for extramedullary hematopoiesis  JAK 2 inhibition- Ruxolitinib (Jakafi ) a specific JAK-STAT pathway inhibitor
  • 34. CRhange in SpRleen Volume. Verstovsek S et al. N Engl J Med 2012;366:799- 807. Verstovsek S et al. NEJM 2012;366:799-807. Change in Spleen Volume
  • 35. Change inChange in Symptom Scores Symptom Scores. Verstovsek S et al. N Engl J Med 2012;366:799-807. Verstovsek S et al. NEJM 2012;366:799-807.
  • 36.  Most common MPD, 2nd most common leukemia in adults, 15-20% of cases  Incidence is 1-2 cases/100,000/year  Median age at diagnosis 50-60 years  3 distinct phases: ◦ Chronic, stable ◦ Accelerated ◦ Blast crisis
  • 37.
  • 38.
  • 39.  Elevated granulocyte count, mostly mature but with some left shift  Increased basophils  Splenomegaly  Increased platelets  Single genetic change
  • 40.
  • 41. MD Anderson*  PB blasts>15%PB blasts + pro>30 %  PB baso>20%  Platelets <100,000/µL not related to tx  Cytogenetic evolution WHO  PB or BM blasts 10-19% PB basophils>20%  Platelets <100,000/µL, unrelated to tx  Cytogenetic evolution  Platelets >1,000,000/µL unresponsive to therapy  Progressive splenomegaly and increasing WBC unresponsive to therapy
  • 42.  ≥20 percent peripheral blood or bone marrow blasts. (70% myeloid, 20% lymphoid, undifferentiated)  Large foci or clusters of blasts on the bone marrow biopsy.  Presence of extramedullary blastic infiltrates (eg, myeloid sarcoma also known as granulocytic sarcoma or chloroma).
  • 43.  Hydroxyurea  TKI’s: Imatinib, dasatinib, nilitonib, ponatinib  Interferon  Allogeneic stem cell transplant  Radiation  Splenectomy