https://orcid.org/0000-0002-4729-4734
![A 62-year-old healthy man felt unwell with chest pain, shortness of breath, and headaches the previous week. A complete blood count showed the following: hemoglobin, 95 g/L; leukocytes, 3.6 × 109/L; platelets, 41 × 109/L; myelocytes, 0.05 × 109/L; neutrophils, 2.35 × 109/L; blasts, 0.27 × 109/L; and nucleated red blood cells (2 per 100 white blood cells). He had no hepatosplenomegaly or lymphadenopathy, but an elevated lactate dehydrogenase concentration (560 U/L). Peripheral blood (PB) showed a leukoerythroblastosis with minimal anisopoikilocytosis. Flow immunophenotyping of PB showed 25% blasts, which were CD34+/CD117+/CD13+/CD33+/MPO–/CD56+/CD4–/CD41–/CD61–. Aspirate was unsuccessful. Biopsy was hypercellular with panmyelosis, including hyperproliferation of megakaryocytes with occasional hypolobated megakaryocytes, erythroid precursors, granulocytic precursors (panel A; original magnification ×20, hematoxylin and eosin stain), and MF-2 reticulin fibrosis (panel B; original magnification ×20, reticulin stain). Immunohistochemistry showed 40% to 50% CD34+ blasts in small aggregates/intrasinusoidal pattern (panel F; original magnification ×40). CD117/MPO (panel E; original magnification ×40), lysozyme/factor 8 (panel C; original magnification ×40), and E-cadherin/spectrin (panel D; original magnification ×40) confirmed the panmyelosis. PML/RARA, RUNX1/RUNX1T1, CBFB-MYH11, BCR/ABL1, and JAK2 on PB were negative. Acute panmyelosis with myelofibrosis (APMF) was contemplated initially. A PB cytogenetic analysis showed 50,XY,-3,-5,-7,+8,add(11)(q14-22),del(12)(p1?2),+21,+22,+mar1,+mar3,+mar4[5]/50,idem,-4,del(6)(q1?2?q25-27),-mar3,+mar5,+mar6[cp4]/46,XY[1]. These findings were consistent with acute myeloid leukemia with myelodysplasia-related changes (AML-MRC) per 2008 and 2016 World Health Organization criteria. / The distinction between AML-MRC and APMF can be very challenging, even with cytogenetics available, because both may have complex karyotypes; the presence of −5/del(5q) and/or −7/del(7q) confirms the diagnosis of AML-MRC as opposed to APMF. This case highlights the importance of PB cytogenetics in the context of dry tap due to fibrosis.](https://ash.silverchair-cdn.com/ash/content_public/journal/blood/130/15/10.1182_blood-2017-06-793554/4/m_blood793554f1.jpeg?Expires=1722451515&Signature=o2yf1ZR9FkW919niYYxYxWqszKevYXxhYJAMLerNWYftQhBKW6lFfxEtHPcCvOC2EKA0LNLa-fH1~MHjw3gorRUvzi6v1j4NcRjEnWg8WGjHBG-ZUKrwD6Jh2xypsoHZ9UYGhmyjuJzSmrOD7aK3AwFxyT~z2XiH~3tyTKQbkAg~Wo1xGPkm6gh70hqDbKgJfCsrXbl4NUhAIVsS4-FkDaOBCRLu0iHxApL7DgSgJG1DG7AXhCFt6~xdh2X4sCxXuWeUP9oGDt1Bm9dgLulxQCEu3crUD-GRD-x8EY5P2JaNO7sA-zMX8EcmY9Fj5o1pscuAJo2QYgL3o3dqQVztdg__&Key-Pair-Id=APKAIE5G5CRDK6RD3PGA)
A 62-year-old healthy man felt unwell with chest pain, shortness of breath, and headaches the previous week. A complete blood count showed the following: hemoglobin, 95 g/L; leukocytes, 3.6 × 109/L; platelets, 41 × 109/L; myelocytes, 0.05 × 109/L; neutrophils, 2.35 × 109/L; blasts, 0.27 × 109/L; and nucleated red blood cells (2 per 100 white blood cells). He had no hepatosplenomegaly or lymphadenopathy, but an elevated lactate dehydrogenase concentration (560 U/L). Peripheral blood (PB) showed a leukoerythroblastosis with minimal anisopoikilocytosis. Flow immunophenotyping of PB showed 25% blasts, which were CD34+/CD117+/CD13+/CD33+/MPO–/CD56+/CD4–/CD41–/CD61–. Aspirate was unsuccessful. Biopsy was hypercellular with panmyelosis, including hyperproliferation of megakaryocytes with occasional hypolobated megakaryocytes, erythroid precursors, granulocytic precursors (panel A; original magnification ×20, hematoxylin and eosin stain), and MF-2 reticulin fibrosis (panel B; original magnification ×20, reticulin stain). Immunohistochemistry showed 40% to 50% CD34+ blasts in small aggregates/intrasinusoidal pattern (panel F; original magnification ×40). CD117/MPO (panel E; original magnification ×40), lysozyme/factor 8 (panel C; original magnification ×40), and E-cadherin/spectrin (panel D; original magnification ×40) confirmed the panmyelosis. PML/RARA, RUNX1/RUNX1T1, CBFB-MYH11, BCR/ABL1, and JAK2 on PB were negative. Acute panmyelosis with myelofibrosis (APMF) was contemplated initially. A PB cytogenetic analysis showed 50,XY,-3,-5,-7,+8,add(11)(q14-22),del(12)(p1?2),+21,+22,+mar1,+mar3,+mar4[5]/50,idem,-4,del(6)(q1?2?q25-27),-mar3,+mar5,+mar6[cp4]/46,XY[1]. These findings were consistent with acute myeloid leukemia with myelodysplasia-related changes (AML-MRC) per 2008 and 2016 World Health Organization criteria.
The distinction between AML-MRC and APMF can be very challenging, even with cytogenetics available, because both may have complex karyotypes; the presence of −5/del(5q) and/or −7/del(7q) confirms the diagnosis of AML-MRC as opposed to APMF. This case highlights the importance of PB cytogenetics in the context of dry tap due to fibrosis.
A 62-year-old healthy man felt unwell with chest pain, shortness of breath, and headaches the previous week. A complete blood count showed the following: hemoglobin, 95 g/L; leukocytes, 3.6 × 109/L; platelets, 41 × 109/L; myelocytes, 0.05 × 109/L; neutrophils, 2.35 × 109/L; blasts, 0.27 × 109/L; and nucleated red blood cells (2 per 100 white blood cells). He had no hepatosplenomegaly or lymphadenopathy, but an elevated lactate dehydrogenase concentration (560 U/L). Peripheral blood (PB) showed a leukoerythroblastosis with minimal anisopoikilocytosis. Flow immunophenotyping of PB showed 25% blasts, which were CD34+/CD117+/CD13+/CD33+/MPO–/CD56+/CD4–/CD41–/CD61–. Aspirate was unsuccessful. Biopsy was hypercellular with panmyelosis, including hyperproliferation of megakaryocytes with occasional hypolobated megakaryocytes, erythroid precursors, granulocytic precursors (panel A; original magnification ×20, hematoxylin and eosin stain), and MF-2 reticulin fibrosis (panel B; original magnification ×20, reticulin stain). Immunohistochemistry showed 40% to 50% CD34+ blasts in small aggregates/intrasinusoidal pattern (panel F; original magnification ×40). CD117/MPO (panel E; original magnification ×40), lysozyme/factor 8 (panel C; original magnification ×40), and E-cadherin/spectrin (panel D; original magnification ×40) confirmed the panmyelosis. PML/RARA, RUNX1/RUNX1T1, CBFB-MYH11, BCR/ABL1, and JAK2 on PB were negative. Acute panmyelosis with myelofibrosis (APMF) was contemplated initially. A PB cytogenetic analysis showed 50,XY,-3,-5,-7,+8,add(11)(q14-22),del(12)(p1?2),+21,+22,+mar1,+mar3,+mar4[5]/50,idem,-4,del(6)(q1?2?q25-27),-mar3,+mar5,+mar6[cp4]/46,XY[1]. These findings were consistent with acute myeloid leukemia with myelodysplasia-related changes (AML-MRC) per 2008 and 2016 World Health Organization criteria.
The distinction between AML-MRC and APMF can be very challenging, even with cytogenetics available, because both may have complex karyotypes; the presence of −5/del(5q) and/or −7/del(7q) confirms the diagnosis of AML-MRC as opposed to APMF. This case highlights the importance of PB cytogenetics in the context of dry tap due to fibrosis.
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