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Chronic myelomonocytic leukemia

March 16, 2024

Chronic myelomonocytic leukemia (CMML) is a type of leukemia, which are cancers of the blood-forming cells of the bone marrow. In adults, blood cells are formed in the bone marrow, by a process that is known as haematopoiesis. In CMML, there are increased numbers of monocytes and immature blood cells (blasts) in the peripheral blood and bone marrow, as well as abnormal looking cells (dysplasia) in at least one type of blood cell.[1]

Chronic myelomonocytic leukemia
Peripheral blood film of CMML. Monocytosis and the presence of myelocytes, metamyelocytes and promyelocytes is typical of CMML.
SpecialtyHaematology, oncology
CausesEnvironmental carcinogens, ionising radiation, cytotoxic agents
Diagnostic methodBlood film, genetic testing
FrequencyLess than 1 per 100,000 per year

CMML shows characteristics of a myelodysplastic syndrome (MDS); a disorder that produces abnormal looking blood cells, and a myeloproliferative neoplasm (MPN); a disorder characterised by the overproduction of blood cells. For this reason, CMML was reclassified as a MDS/MPN overlap disorder in 2002.[2] For a diagnosis of CMML, the World Health Organization (WHO) states that the blood monocyte count must be >1x109/L, no Philadelphia chromosome or mutations in the PDGFRA or PDGFRB gene should be present, the blast count must be <20% and dysplasia of at least one lineage of myeloid blood cell should be present.[3]

Azacitidine is a drug used to treat CMML and is approved by the Food and Drug Administration (FDA) and the European Medicines Agency. Stem cell transplant is also used to treat CMML, and involves the transplantation of donor haematopoietic stem cells into the recipient. Blood transfusion and erythropoietin are used to treat disease associated anaemia.[4][5][6]

Signs and symptoms edit

One of the most common signs of CMML is splenomegaly, found in approximately half of cases. Other less frequent signs and symptoms consist of anaemia, fever, weight loss, night sweats, infection, bleeding, synovitis, lymphadenopathy, skin rashes, pleural effusion, pericardial effusion and peritoneal effusion.[7][8][9]

Cause edit

Although the cause of CMML is unknown, environmental carcinogens, ionising radiation and cytotoxic agents may have a role in causing disease.[8] Approximately one third of cases of MDS with a monocyte count of >10% and <1x109/L will progress to CMML.[10]

Pathogenesis edit

With a high rate of Ras mutation in CMML, deregulation of this signalling pathway has been linked to the pathogenesis of the disease. Tumour necrosis factor, GM-CSF, interleukin-3, interleukin-4, interleukin-6, and interleukin-10 may have a role in hyperproliferative CMML cells. These cytokines can stimulate the growth of CMML in vitro.[11] Hypermethylation of cytosine residues (usually in the promoter regions of genes) occurs in many malignancies to regulate gene expression. One commonly hypermethylated gene in CMML is p15INK4b, a gene involved in cell cycle regulation.[4]

Genetic mutations edit

Clonal genetic abnormalities are common in CMML but they are not specific for diagnosis of the disease. The most common found are the 8+, −7/del (7q) and structural 12p abnormalities.[8] KRAS and NRAS are mutated in 25–40% of the cases of CMML. The Jak2 V617F mutation is found in 10% of cases. Mutations in transcription factors such as RUNX1, CEBPA, NPM1 and WT1 have been found in up to 30% of cases. Mutations of CBL are found in approximately 5–18% of cases.[3] Mutations in the TET2 gene are found in approximately 40–50% of CMML.[12] Inactivating mutations in one of the two parental GATA2 genes lead to a reduction, i.e. a haploinsufficiency, in the cellular levels of the gene's product, the GATA2 transcription factor, and thereby to a rare autosomal dominant genetic disease, GATA2 deficiency. This disease is associated with a highly variable set of disorders including the myelodysplastic syndrome, acute myeloid leukemia, and CMML. GATA2-deficiency-induced CMML, like other types of CMML, is commonly preceded by monocytosis.[13][14]

Diagnosis edit

Blood films display a range of abnormalities. A monocyte count of >1x109/L is essential for a diagnosis of CMML. Other features may include; leukocytosis (50% of cases); left shift and dysplasia of monocytes and granulocytes; presence of metamyelocytes, myelocytes and promonocytes; monocytes with hypersegmented/abnormal shaped nuclei, increased cytoplasmic basophilia and/or the presence of cytoplasmic granules; eosinophilia (in cases of CMML with eosinophilia); and spherocytosis (in cases of direct Coombs test, DCT, positive haemolytic anaemia). Platelet counts may be reduced, increased or normal.[7][15][16] Haemoglobin levels are usually reduced with normocytic and normochromic red blood cells. Autoantibodies and cold agglutinins may be present and 10% of CMML is DCT positive.[7][9]Bone marrow aspirates will display hypercellularity with increased counts of granulocytic and monocytic cells.[1] Bone marrow core biopsies may show a predominance of myelocytic and monocytic cells, abnormal localisation of immature precursors and dysplastic megakaryocytes.[1] Monocytic nodules are a common feature in biopsies.[16]

The phenotypical characteristics of CMML are; CD11b, CD11c, CD14, CD33, CD45 and CD64 seen in 100% of cases; CD13 found in 95% of cases; CD4 found in 76% of cases; HLA-DR found in 71% of cases; CD56 found in 53% of cases; CD2 found in 34% of cases; CD16 found in 29% of cases; CD10 found in 28% of cases; CD23 and CD7 found in 9% of cases; and CD117 found in 5% of cases.[17]

Classification edit

 
Haematopoiesis. The two lineages of myeloid and lymphoid cells are formed from haematopoietic stem cells.

Leukemia subtypes are categorised into single clinical entities so that they can be diagnosed and treated appropriately. Leukaemias are subdivided into lymphoid and myeloid neoplasms, depending on which bone marrow cells are cancerous. The myeloid neoplasms contain acute and chronic leukemias, myelodysplastic syndromes (MDSs) and myeloproliferative neoplasms (MPNs). MPNs are characterised by increased production of myeloid blood cells, with a higher than normal number of mature cells. Unlike MPNs, MDSs have a dysfunctional production of myeloid cells with a reduced number of mature cells. Many of the cells produced in MDS are abnormal looking, known as dysplasia. CMML shows characteristics of both groups and thus is a difficult disease to categorise.[7][18]

FAB classification edit

The French-American-British (FAB) classification system was published in 1976 to classify the leukaemias. It placed CMML into the category of MDS, along with the refractory anaemia, refractory anaemia with ring sideroblasts, refractory anaemia with excess blasts and refractory anaemia with excess blasts in transformation. The system does have clinical utility; however factors such as cytogenetic status are not within the remit of the classification. For this reason, many disease entities in these groups show a great deal of heterogeneity.[18][19]

WHO classification edit

In 2001, the WHO Classification of Myeloid Neoplasms was published, classifying CMML into a new group of diseases, the myelodysplastic/myeloproliferative neoplasms (MDS/MPN), reflecting the disease's neoplastic nature. Other diseases in this category are juvenile myelomonocytic leukaemia, atypical CML; BCR-ABL1 negative and MDS/MPD unclassifiable. These MDS/MPN overlap syndromes have effective production of some lineages of blood cells, but show ineffective proliferation of other lineages. The 2008 revision of the classification moved cases of CMML with PDGFR gene translocations to a new group, myeloid/lymphoid neoplasms with eosinophilia with abnormalities of PDGFRA, PDGFRB or FGFR1.[2][7][20]

Diagnostic criteria edit

FAB criteria edit

The FAB criteria for diagnosis are as follows:[21]

  • Monocyte count >1x109/L
  • 0–19% blasts in bone marrow
  • <5% blasts in peripheral blood

The FAB also arbitrarily categorises CMML into myelodysplastic-like and myeloproliferative-like groups. A white blood count of 13x109 is used as a cut-off to differentiate the two.[12]

WHO criteria edit

The WHO criteria for diagnosis are as follows:[3]

  • Persistent peripheral blood monocytosis with counts >1x109/L
  • No Philadelphia chromosome or BCR-ABL1 fusion gene
  • No rearrangement of PDGFRA or PDGFRB gene
  • <20% myeloblasts, monoblasts and promonocytes in peripheral blood or bone marrow
  • Dysplasia in one or more of the myeloid lineages; if myelodysplasia is absent or minimal then a diagnosis of CMML can be made if other requirements are met and:
    • A molecular genetic abnormality is present in haematopoietic cells, or
    • Monocytosis present for ≥3 months and other causes of monocytosis have been ruled out

WHO defined CMML has two main subsets, CMML-1 and CMML-2. CMML-1 is diagnosed if myeloblasts, monoblasts and promonocytes are <5% of peripheral blood and <10% of bone marrow. CMML-2 is diagnosed if:

  • Myeloblasts, monoblasts or promonocytes are 5-19% in blood, or
  • Myeloblasts, monoblasts or promonocytes are 10-19% in bone marrow, or
  • Auer rods are present

CMML-1 and CMML-2 can be additionally grouped as CMML-1 or CMML-2 with eosinophilia. These are diagnosed if the above criteria are met and the blood eosinophil count is >1.5x109/L.[8]

Presence of two or more phenotypic abnormalities can aid a diagnosis of CMML in the absence of identifying cytogenetic or dysplastic features. These can include the expression of CD56 and/or CD2, or under-expression of HLA-DR.[3]

Prognosis edit

Factors affecting prognosis edit

CMML-2 has a reduced overall survival as compared with CMML-1, with median survivals of 15 and 20 months, respectively. Myeloproliferative CMML (>13x109 monocytes/L) has a reduced survival compared with myelodysplastic CMML. A platelet count of <100 x109/L reduces overall survival. A haemoglobin level of <10g/dL has a reduced overall survival. Some cytogenetic abnormalities have implications on the prognosis of CMML. Normal karyotypes or the single loss of the Y chromosome have low risk prognoses. Trisomy 8, chromosome 7 abnormalities and complex karyotypes comprise a high risk group. Other cytogenetic abnormalities have intermediate prognoses. Somatic mutations in genes such as ASXL1 and EZH2 are associated with a poor prognosis.[12]

CMML has a 20–30% chance of transformation to AML, a lower rate than other similar diseases. The CMML-2 subtype is associated with increased risk of transformation and ASXL1 and RUNX1 mutations also increase the risk of transition to AML.[12][22][23]

Scoring systems edit

IPSS edit

The International Prognostic Scoring System (IPSS) was developed in the mid-1990s to assess the prognosis of MDS patients. This system stratifies cases into 2 groups; a lower-risk group (sub divided into low and intermediate-1) and a higher risk (subdivided into intermediate-2 and high). It uses the blast percentage, number of cytopenias and bone marrow cytogenetics data to place cases of CMML into these groups. Due to the scoring system being developed for MDS, the more myeloproliferative cases of CMML (WBC >13x109) are excluded from the scoring system. Although the IPSS scoring system is used clinically, there is a high variability in each group. For this reason, new modalities for assessing prognosis in MDS (and CMML) are being developed.[12][24]

MD Anderson Prognostic Scoring System edit

A new method developed using data from the M.D. Anderson Cancer Center found that a haemoglobin level of <12g/dL, total circulating lymphocyte count of >2.5 x 109/L, >0% immature myeloid cells, >10% bone marrow blasts causes a reduced overall survival. This data allows cases of CMML to be stratified into low, intermediate-1, intermediate-2 and high risk groups. These groups have median survival times of 24, 15, 8 and 5 months respectively.[25][26]

The Düsseldorf score edit

The Düsseldorf score stratifies cases using four categories, giving one point for each; bone marrow blasts ≥5%, LDH >200U/L, haemoglobin ≤9g/dL and a platelet count ≤100,000/uL. A score of 0 indicates a low risk group' 1-2 indicates an intermediate risk group and 3-4 indicates a high risk group. The cumulative 2 year survival of scores 0, 1-2 and 3-4 is 91%, 52% and 9%; and risk of AML transformation is 0%, 19% and 54% respectively.[10]

Treatment edit

The treatment of CMML remains challenging due to the lack of clinical trials investigating the disease as its own clinical entity. It is often grouped with MDS in clinical trials, and for this reason the treatment of CMML is very similar to that of MDS. Most cases are dealt with as supportive rather than curative because most therapies do not effectively increase survival. Indications for treatment include the presence of B symptoms, symptomatic organ involvement, increasing blood counts, hyperleukocytosis, leukostasis and/or worsening cytopenias.[6][10]

Blood transfusions and erythropoietin administration are used to raise haemoglobin levels in cases with anemia.[6]

Azacitidine is a drug approved by the U.S. Food and Drug Administration (FDA) for the treatment of CMML and by the European Medicines Agency (EMA) for high risk non-proliferative CMML with 10–19% marrow blasts. It is a cytidine analogue that causes hypomethylation of DNA by inhibition of DNA methyltransferase. Decitabine is a similar drug to azacitidine and is approved by the FDA for treatments of all subtypes of MDS, including CMML. Hydroxyurea is a chemotherapy that is used in the myeloproliferative form of CMML to reduce cell numbers.[4][10][12] Decitabine/cedazuridine (Inqovi) is a fixed-dosed combination medication for the treatment of adults with myelodysplastic syndromes (MDS) and chronic myelomonocytic leukemia (CMML) that was approved for use in the United States in July 2020.[27]

Hematopoietic stem cell transplantation remains the only curative treatment for CMML. However, due to the late age of onset and presence of other illnesses, this form of treatment is often not possible.[5][28]

Epidemiology edit

There have been few individual epidemiological studies of CMML, due to the difficulty in the disease classification. CMML has an estimated incidence of less than 1 per 100,000 persons per year.[12] The median age of diagnosis is 65–75. CMML has a propensity for males rather than females, at a ratio of 1.5–3:1.[8]

References edit

  1. ^ a b c Foucar K (August 2009). "Myelodysplastic/myeloproliferative neoplasms". Am. J. Clin. Pathol. 132 (2): 281–9. doi:10.1309/AJCPJ71PTVIKGEVT. PMID 19605822.
  2. ^ a b Vardiman JW, Harris NL, Brunning RD (October 2002). "The World Health Organization (WHO) classification of the myeloid neoplasms". Blood. 100 (7): 2292–302. doi:10.1182/blood-2002-04-1199. PMID 12239137.
  3. ^ a b c d Vardiman J, Hyjek E (2011). "World health organization classification, evaluation, and genetics of the myeloproliferative neoplasm variants". Hematology. 2011: 250–6. doi:10.1182/asheducation-2011.1.250. PMID 22160042.
  4. ^ a b c McCormack, SE; Warlick, ED (Sep 7, 2010). "Epigenetic approaches in the treatment of myelodysplastic syndromes: clinical utility of azacitidine". OncoTargets and Therapy. 3: 157–65. doi:10.2147/OTT.S5852. PMC 2939768. PMID 20856790.
  5. ^ a b Robert J. Soiffer (17 November 2008). Hematopoietic Stem Cell Transplantation. Springer. ISBN 978-1-934115-05-3. Retrieved 23 September 2012.
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  8. ^ a b c d e Pathology and Genetics of Haemo (World Health Organization Classification of Tumours S.). Oxford Univ Pr. 2003. ISBN 978-92-832-2411-2.
  9. ^ a b Paul Moss; Victor Hoffbrand (2011). Essential Haematology, Includes FREE Desktop Edition (Essentials). Wiley-Blackwell. ISBN 978-1-4051-9890-5.
  10. ^ a b c d Viktoria Faber; Richard Greil; Lisa Pleyer; Daniel Neureiter (2010). Chronic Myeloid Neoplasias and Clonal Overlap Syndromes: Epidemiology, Pathophysiology and Treatment Options. Berlin: Springer. ISBN 978-3-211-79891-1.
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  13. ^ Crispino JD, Horwitz MS (April 2017). "GATA factor mutations in hematologic disease". Blood. 129 (15): 2103–2110. doi:10.1182/blood-2016-09-687889. PMC 5391620. PMID 28179280.
  14. ^ Hirabayashi S, Wlodarski MW, Kozyra E, Niemeyer CM (August 2017). "Heterogeneity of GATA2-related myeloid neoplasms". International Journal of Hematology. 106 (2): 175–182. doi:10.1007/s12185-017-2285-2. PMID 28643018.
  15. ^ Hirschmann, Jan V.; Tkachuk, Douglas C.; Wintrobe, Maxwell Myer (2007). Wintrobe's atlas of clinical hematology. Philadelphia: Wolters Kluwer Health/Lippincott Williams & Wilkins. ISBN 978-0-7817-7023-1.
  16. ^ a b Wayne W. Grody; Naeim, Faramarz (2008). Hematopathology: morphology, immunophenotype, cytogenetics, and molecular approaches. Amsterdam: Elsevier/Academic Press. ISBN 978-0-12-370607-2.
  17. ^ Foxwell Nathan Emmons; Wojciech Gorczyca; James Weisberger (2004). An Atlas of Differential Diagnosis in Neoplastic Hematopathology. Washington, DC: Taylor & Francis. ISBN 978-1-84214-247-9.
  18. ^ a b Bhargava R, Dalal BI (2010). "Two steps forward, one step back: 4th WHO classification of myeloid neoplasms (2008)". Indian J Pathol Microbiol. 53 (3): 391–4. doi:10.4103/0377-4929.68240. PMID 20699489.
  19. ^ Turgeon, Mary Louise (1999). Clinical hematology: theory and procedures. Hagerstwon, MD: Lippincott Williams & Wilkins. pp. 321–322. ISBN 978-0-316-85623-2.
  20. ^ Tsongalis, Gregory J.; Coleman, William L. (2009). MOLECULAR PATHOLOGY: THE MOLECULAR BASIS OF HUMAN DISEASE; ED. BY WILLIAM B. COLEMAN. Amsterdam: Elsevier Academic Press. ISBN 978-0-12-374419-7.
  21. ^ Bennett JM, Catovsky D, Daniel MT, et al. (June 1982). "Proposals for the classification of the myelodysplastic syndromes". Br. J. Haematol. 51 (2): 189–99. CiteSeerX 10.1.1.630.8355. doi:10.1111/j.1365-2141.1982.tb02771.x. PMID 6952920. S2CID 293823.
  22. ^ William G. Finn; LoAnn C. Peterson (31 May 2004). Hematopathology in Oncology. Springer. pp. 33–. ISBN 978-1-4020-7919-1. Retrieved 23 September 2012.
  23. ^ Barbara J. Bain (2003). Chronic Myeloproliferative Disorders: Cytogenetic and Molecular Genetic Abnormalities. Karger Publishers. pp. 72–. ISBN 978-3-8055-7307-8. Retrieved 23 September 2012.
  24. ^ Greenberg P, Cox C, LeBeau MM, et al. (March 1997). "International scoring system for evaluating prognosis in myelodysplastic syndromes". Blood. 89 (6): 2079–88. doi:10.1182/blood.V89.6.2079. PMID 9058730.
  25. ^ Garcia-Manero G (2010). "Prognosis of myelodysplastic syndromes". Hematology. 2010: 330–7. doi:10.1182/asheducation-2010.1.330. PMID 21239815.
  26. ^ Onida F, Kantarjian HM, Smith TL, et al. (February 2002). "Prognostic factors and scoring systems in chronic myelomonocytic leukemia: a retrospective analysis of 213 patients". Blood. 99 (3): 840–9. doi:10.1182/blood.V99.3.840. PMID 11806985. S2CID 1310629.
  27. ^ "FDA Approves New Therapy for Myelodysplastic Syndromes (MDS) That Can Be Taken at Home". U.S. Food and Drug Administration (FDA) (Press release). 7 July 2020. Retrieved 7 July 2020.   This article incorporates text from this source, which is in the public domain.
  28. ^ Bacher U, Haferlach T, Schnittger S, Kreipe H, Kröger N (March 2011). "Recent advances in diagnosis, molecular pathology and therapy of chronic myelomonocytic leukaemia". Br J Haematol. 153 (2): 149–67. doi:10.1111/j.1365-2141.2011.08631.x. PMID 21401573.

External links edit

March 16, 2024
chronic, myelomonocytic, leukemia, cmml, type, leukemia, which, cancers, blood, forming, cells, bone, marrow, adults, blood, cells, formed, bone, marrow, process, that, known, haematopoiesis, cmml, there, increased, numbers, monocytes, immature, blood, cells, . Chronic myelomonocytic leukemia CMML is a type of leukemia which are cancers of the blood forming cells of the bone marrow In adults blood cells are formed in the bone marrow by a process that is known as haematopoiesis In CMML there are increased numbers of monocytes and immature blood cells blasts in the peripheral blood and bone marrow as well as abnormal looking cells dysplasia in at least one type of blood cell 1 Chronic myelomonocytic leukemiaPeripheral blood film of CMML Monocytosis and the presence of myelocytes metamyelocytes and promyelocytes is typical of CMML SpecialtyHaematology oncologyCausesEnvironmental carcinogens ionising radiation cytotoxic agentsDiagnostic methodBlood film genetic testingFrequencyLess than 1 per 100 000 per yearCMML shows characteristics of a myelodysplastic syndrome MDS a disorder that produces abnormal looking blood cells and a myeloproliferative neoplasm MPN a disorder characterised by the overproduction of blood cells For this reason CMML was reclassified as a MDS MPN overlap disorder in 2002 2 For a diagnosis of CMML the World Health Organization WHO states that the blood monocyte count must be gt 1x109 L no Philadelphia chromosome or mutations in the PDGFRA or PDGFRB gene should be present the blast count must be lt 20 and dysplasia of at least one lineage of myeloid blood cell should be present 3 Azacitidine is a drug used to treat CMML and is approved by the Food and Drug Administration FDA and the European Medicines Agency Stem cell transplant is also used to treat CMML and involves the transplantation of donor haematopoietic stem cells into the recipient Blood transfusion and erythropoietin are used to treat disease associated anaemia 4 5 6 Contents 1 Signs and symptoms 2 Cause 3 Pathogenesis 3 1 Genetic mutations 4 Diagnosis 4 1 Classification 4 1 1 FAB classification 4 1 2 WHO classification 4 2 Diagnostic criteria 4 2 1 FAB criteria 4 2 2 WHO criteria 5 Prognosis 5 1 Factors affecting prognosis 5 2 Scoring systems 5 2 1 IPSS 5 2 2 MD Anderson Prognostic Scoring System 5 2 3 The Dusseldorf score 6 Treatment 7 Epidemiology 8 References 9 External linksSigns and symptoms editOne of the most common signs of CMML is splenomegaly found in approximately half of cases Other less frequent signs and symptoms consist of anaemia fever weight loss night sweats infection bleeding synovitis lymphadenopathy skin rashes pleural effusion pericardial effusion and peritoneal effusion 7 8 9 Cause editAlthough the cause of CMML is unknown environmental carcinogens ionising radiation and cytotoxic agents may have a role in causing disease 8 Approximately one third of cases of MDS with a monocyte count of gt 10 and lt 1x109 L will progress to CMML 10 Pathogenesis editWith a high rate of Ras mutation in CMML deregulation of this signalling pathway has been linked to the pathogenesis of the disease Tumour necrosis factor GM CSF interleukin 3 interleukin 4 interleukin 6 and interleukin 10 may have a role in hyperproliferative CMML cells These cytokines can stimulate the growth of CMML in vitro 11 Hypermethylation of cytosine residues usually in the promoter regions of genes occurs in many malignancies to regulate gene expression One commonly hypermethylated gene in CMML is p15INK4b a gene involved in cell cycle regulation 4 Genetic mutations edit Clonal genetic abnormalities are common in CMML but they are not specific for diagnosis of the disease The most common found are the 8 7 del 7q and structural 12p abnormalities 8 KRAS and NRAS are mutated in 25 40 of the cases of CMML The Jak2 V617F mutation is found in 10 of cases Mutations in transcription factors such as RUNX1 CEBPA NPM1 and WT1 have been found in up to 30 of cases Mutations of CBL are found in approximately 5 18 of cases 3 Mutations in the TET2 gene are found in approximately 40 50 of CMML 12 Inactivating mutations in one of the two parental GATA2 genes lead to a reduction i e a haploinsufficiency in the cellular levels of the gene s product the GATA2 transcription factor and thereby to a rare autosomal dominant genetic disease GATA2 deficiency This disease is associated with a highly variable set of disorders including the myelodysplastic syndrome acute myeloid leukemia and CMML GATA2 deficiency induced CMML like other types of CMML is commonly preceded by monocytosis 13 14 Diagnosis editBlood films display a range of abnormalities A monocyte count of gt 1x109 L is essential for a diagnosis of CMML Other features may include leukocytosis 50 of cases left shift and dysplasia of monocytes and granulocytes presence of metamyelocytes myelocytes and promonocytes monocytes with hypersegmented abnormal shaped nuclei increased cytoplasmic basophilia and or the presence of cytoplasmic granules eosinophilia in cases of CMML with eosinophilia and spherocytosis in cases of direct Coombs test DCT positive haemolytic anaemia Platelet counts may be reduced increased or normal 7 15 16 Haemoglobin levels are usually reduced with normocytic and normochromic red blood cells Autoantibodies and cold agglutinins may be present and 10 of CMML is DCT positive 7 9 Bone marrow aspirates will display hypercellularity with increased counts of granulocytic and monocytic cells 1 Bone marrow core biopsies may show a predominance of myelocytic and monocytic cells abnormal localisation of immature precursors and dysplastic megakaryocytes 1 Monocytic nodules are a common feature in biopsies 16 The phenotypical characteristics of CMML are CD11b CD11c CD14 CD33 CD45 and CD64 seen in 100 of cases CD13 found in 95 of cases CD4 found in 76 of cases HLA DR found in 71 of cases CD56 found in 53 of cases CD2 found in 34 of cases CD16 found in 29 of cases CD10 found in 28 of cases CD23 and CD7 found in 9 of cases and CD117 found in 5 of cases 17 Classification edit nbsp Haematopoiesis The two lineages of myeloid and lymphoid cells are formed from haematopoietic stem cells Leukemia subtypes are categorised into single clinical entities so that they can be diagnosed and treated appropriately Leukaemias are subdivided into lymphoid and myeloid neoplasms depending on which bone marrow cells are cancerous The myeloid neoplasms contain acute and chronic leukemias myelodysplastic syndromes MDSs and myeloproliferative neoplasms MPNs MPNs are characterised by increased production of myeloid blood cells with a higher than normal number of mature cells Unlike MPNs MDSs have a dysfunctional production of myeloid cells with a reduced number of mature cells Many of the cells produced in MDS are abnormal looking known as dysplasia CMML shows characteristics of both groups and thus is a difficult disease to categorise 7 18 FAB classification edit The French American British FAB classification system was published in 1976 to classify the leukaemias It placed CMML into the category of MDS along with the refractory anaemia refractory anaemia with ring sideroblasts refractory anaemia with excess blasts and refractory anaemia with excess blasts in transformation The system does have clinical utility however factors such as cytogenetic status are not within the remit of the classification For this reason many disease entities in these groups show a great deal of heterogeneity 18 19 WHO classification edit In 2001 the WHO Classification of Myeloid Neoplasms was published classifying CMML into a new group of diseases the myelodysplastic myeloproliferative neoplasms MDS MPN reflecting the disease s neoplastic nature Other diseases in this category are juvenile myelomonocytic leukaemia atypical CML BCR ABL1 negative and MDS MPD unclassifiable These MDS MPN overlap syndromes have effective production of some lineages of blood cells but show ineffective proliferation of other lineages The 2008 revision of the classification moved cases of CMML with PDGFR gene translocations to a new group myeloid lymphoid neoplasms with eosinophilia with abnormalities of PDGFRA PDGFRB or FGFR1 2 7 20 Diagnostic criteria edit FAB criteria edit The FAB criteria for diagnosis are as follows 21 Monocyte count gt 1x109 L 0 19 blasts in bone marrow lt 5 blasts in peripheral bloodThe FAB also arbitrarily categorises CMML into myelodysplastic like and myeloproliferative like groups A white blood count of 13x109 is used as a cut off to differentiate the two 12 WHO criteria edit The WHO criteria for diagnosis are as follows 3 Persistent peripheral blood monocytosis with counts gt 1x109 L No Philadelphia chromosome or BCR ABL1 fusion gene No rearrangement of PDGFRA or PDGFRB gene lt 20 myeloblasts monoblasts and promonocytes in peripheral blood or bone marrow Dysplasia in one or more of the myeloid lineages if myelodysplasia is absent or minimal then a diagnosis of CMML can be made if other requirements are met and A molecular genetic abnormality is present in haematopoietic cells or Monocytosis present for 3 months and other causes of monocytosis have been ruled outWHO defined CMML has two main subsets CMML 1 and CMML 2 CMML 1 is diagnosed if myeloblasts monoblasts and promonocytes are lt 5 of peripheral blood and lt 10 of bone marrow CMML 2 is diagnosed if Myeloblasts monoblasts or promonocytes are 5 19 in blood or Myeloblasts monoblasts or promonocytes are 10 19 in bone marrow or Auer rods are presentCMML 1 and CMML 2 can be additionally grouped as CMML 1 or CMML 2 with eosinophilia These are diagnosed if the above criteria are met and the blood eosinophil count is gt 1 5x109 L 8 Presence of two or more phenotypic abnormalities can aid a diagnosis of CMML in the absence of identifying cytogenetic or dysplastic features These can include the expression of CD56 and or CD2 or under expression of HLA DR 3 Prognosis editFactors affecting prognosis edit CMML 2 has a reduced overall survival as compared with CMML 1 with median survivals of 15 and 20 months respectively Myeloproliferative CMML gt 13x109 monocytes L has a reduced survival compared with myelodysplastic CMML A platelet count of lt 100 x109 L reduces overall survival A haemoglobin level of lt 10g dL has a reduced overall survival Some cytogenetic abnormalities have implications on the prognosis of CMML Normal karyotypes or the single loss of the Y chromosome have low risk prognoses Trisomy 8 chromosome 7 abnormalities and complex karyotypes comprise a high risk group Other cytogenetic abnormalities have intermediate prognoses Somatic mutations in genes such as ASXL1 and EZH2 are associated with a poor prognosis 12 CMML has a 20 30 chance of transformation to AML a lower rate than other similar diseases The CMML 2 subtype is associated with increased risk of transformation and ASXL1 and RUNX1 mutations also increase the risk of transition to AML 12 22 23 Scoring systems edit IPSS edit The International Prognostic Scoring System IPSS was developed in the mid 1990s to assess the prognosis of MDS patients This system stratifies cases into 2 groups a lower risk group sub divided into low and intermediate 1 and a higher risk subdivided into intermediate 2 and high It uses the blast percentage number of cytopenias and bone marrow cytogenetics data to place cases of CMML into these groups Due to the scoring system being developed for MDS the more myeloproliferative cases of CMML WBC gt 13x109 are excluded from the scoring system Although the IPSS scoring system is used clinically there is a high variability in each group For this reason new modalities for assessing prognosis in MDS and CMML are being developed 12 24 MD Anderson Prognostic Scoring System edit A new method developed using data from the M D Anderson Cancer Center found that a haemoglobin level of lt 12g dL total circulating lymphocyte count of gt 2 5 x 109 L gt 0 immature myeloid cells gt 10 bone marrow blasts causes a reduced overall survival This data allows cases of CMML to be stratified into low intermediate 1 intermediate 2 and high risk groups These groups have median survival times of 24 15 8 and 5 months respectively 25 26 The Dusseldorf score edit The Dusseldorf score stratifies cases using four categories giving one point for each bone marrow blasts 5 LDH gt 200U L haemoglobin 9g dL and a platelet count 100 000 uL A score of 0 indicates a low risk group 1 2 indicates an intermediate risk group and 3 4 indicates a high risk group The cumulative 2 year survival of scores 0 1 2 and 3 4 is 91 52 and 9 and risk of AML transformation is 0 19 and 54 respectively 10 Treatment editThe treatment of CMML remains challenging due to the lack of clinical trials investigating the disease as its own clinical entity It is often grouped with MDS in clinical trials and for this reason the treatment of CMML is very similar to that of MDS Most cases are dealt with as supportive rather than curative because most therapies do not effectively increase survival Indications for treatment include the presence of B symptoms symptomatic organ involvement increasing blood counts hyperleukocytosis leukostasis and or worsening cytopenias 6 10 Blood transfusions and erythropoietin administration are used to raise haemoglobin levels in cases with anemia 6 Azacitidine is a drug approved by the U S Food and Drug Administration FDA for the treatment of CMML and by the European Medicines Agency EMA for high risk non proliferative CMML with 10 19 marrow blasts It is a cytidine analogue that causes hypomethylation of DNA by inhibition of DNA methyltransferase Decitabine is a similar drug to azacitidine and is approved by the FDA for treatments of all subtypes of MDS including CMML Hydroxyurea is a chemotherapy that is used in the myeloproliferative form of CMML to reduce cell numbers 4 10 12 Decitabine cedazuridine Inqovi is a fixed dosed combination medication for the treatment of adults with myelodysplastic syndromes MDS and chronic myelomonocytic leukemia CMML that was approved for use in the United States in July 2020 27 Hematopoietic stem cell transplantation remains the only curative treatment for CMML However due to the late age of onset and presence of other illnesses this form of treatment is often not possible 5 28 Epidemiology editThere have been few individual epidemiological studies of CMML due to the difficulty in the disease classification CMML has an estimated incidence of less than 1 per 100 000 persons per year 12 The median age of diagnosis is 65 75 CMML has a propensity for males rather than females at a ratio of 1 5 3 1 8 References edit a b c Foucar K August 2009 Myelodysplastic myeloproliferative neoplasms Am J Clin Pathol 132 2 281 9 doi 10 1309 AJCPJ71PTVIKGEVT PMID 19605822 a b Vardiman JW Harris NL Brunning RD October 2002 The World Health Organization WHO classification of the myeloid neoplasms Blood 100 7 2292 302 doi 10 1182 blood 2002 04 1199 PMID 12239137 a b c d Vardiman J Hyjek E 2011 World health organization classification evaluation and genetics of the myeloproliferative neoplasm variants Hematology 2011 250 6 doi 10 1182 asheducation 2011 1 250 PMID 22160042 a b c McCormack SE Warlick ED Sep 7 2010 Epigenetic approaches in the treatment of myelodysplastic syndromes clinical utility of azacitidine OncoTargets and Therapy 3 157 65 doi 10 2147 OTT S5852 PMC 2939768 PMID 20856790 a b Robert J Soiffer 17 November 2008 Hematopoietic Stem Cell Transplantation Springer ISBN 978 1 934115 05 3 Retrieved 23 September 2012 a b c Bennett JM June 2002 Chronic myelomonocytic leukemia Current Treatment Options in Oncology 3 3 221 3 doi 10 1007 s11864 002 0011 6 PMID 12057067 S2CID 6069664 a b c d e Bain Barbara J 2003 Leukaemia Diagnosis Cambridge MA Blackwell Publishers ISBN 978 1 4051 0661 0 a b c d e Pathology and Genetics of Haemo World Health Organization Classification of Tumours S Oxford Univ Pr 2003 ISBN 978 92 832 2411 2 a b Paul Moss Victor Hoffbrand 2011 Essential Haematology Includes FREE Desktop Edition Essentials Wiley Blackwell ISBN 978 1 4051 9890 5 a b c d Viktoria Faber Richard Greil Lisa Pleyer Daniel Neureiter 2010 Chronic Myeloid Neoplasias and Clonal Overlap Syndromes Epidemiology Pathophysiology and Treatment Options Berlin Springer ISBN 978 3 211 79891 1 Arceci RJ Longley BJ Emanuel PD 2002 Atypical cellular disorders Hematology 2002 297 314 doi 10 1182 asheducation 2002 1 297 PMID 12446429 a b c d e f g Cazzola M Malcovati L Invernizzi R 2011 Myelodysplastic myeloproliferative neoplasms Hematology 2011 264 72 doi 10 1182 asheducation 2011 1 264 PMID 22160044 S2CID 24489846 Crispino JD Horwitz MS April 2017 GATA factor mutations in hematologic disease Blood 129 15 2103 2110 doi 10 1182 blood 2016 09 687889 PMC 5391620 PMID 28179280 Hirabayashi S Wlodarski MW Kozyra E Niemeyer CM August 2017 Heterogeneity of GATA2 related myeloid neoplasms International Journal of Hematology 106 2 175 182 doi 10 1007 s12185 017 2285 2 PMID 28643018 Hirschmann Jan V Tkachuk Douglas C Wintrobe Maxwell Myer 2007 Wintrobe s atlas of clinical hematology Philadelphia Wolters Kluwer Health Lippincott Williams amp Wilkins ISBN 978 0 7817 7023 1 a b Wayne W Grody Naeim Faramarz 2008 Hematopathology morphology immunophenotype cytogenetics and molecular approaches Amsterdam Elsevier Academic Press ISBN 978 0 12 370607 2 Foxwell Nathan Emmons Wojciech Gorczyca James Weisberger 2004 An Atlas of Differential Diagnosis in Neoplastic Hematopathology Washington DC Taylor amp Francis ISBN 978 1 84214 247 9 a b Bhargava R Dalal BI 2010 Two steps forward one step back 4th WHO classification of myeloid neoplasms 2008 Indian J Pathol Microbiol 53 3 391 4 doi 10 4103 0377 4929 68240 PMID 20699489 Turgeon Mary Louise 1999 Clinical hematology theory and procedures Hagerstwon MD Lippincott Williams amp Wilkins pp 321 322 ISBN 978 0 316 85623 2 Tsongalis Gregory J Coleman William L 2009 MOLECULAR PATHOLOGY THE MOLECULAR BASIS OF HUMAN DISEASE ED BY WILLIAM B COLEMAN Amsterdam Elsevier Academic Press ISBN 978 0 12 374419 7 Bennett JM Catovsky D Daniel MT et al June 1982 Proposals for the classification of the myelodysplastic syndromes Br J Haematol 51 2 189 99 CiteSeerX 10 1 1 630 8355 doi 10 1111 j 1365 2141 1982 tb02771 x PMID 6952920 S2CID 293823 William G Finn LoAnn C Peterson 31 May 2004 Hematopathology in Oncology Springer pp 33 ISBN 978 1 4020 7919 1 Retrieved 23 September 2012 Barbara J Bain 2003 Chronic Myeloproliferative Disorders Cytogenetic and Molecular Genetic Abnormalities Karger Publishers pp 72 ISBN 978 3 8055 7307 8 Retrieved 23 September 2012 Greenberg P Cox C LeBeau MM et al March 1997 International scoring system for evaluating prognosis in myelodysplastic syndromes Blood 89 6 2079 88 doi 10 1182 blood V89 6 2079 PMID 9058730 Garcia Manero G 2010 Prognosis of myelodysplastic syndromes Hematology 2010 330 7 doi 10 1182 asheducation 2010 1 330 PMID 21239815 Onida F Kantarjian HM Smith TL et al February 2002 Prognostic factors and scoring systems in chronic myelomonocytic leukemia a retrospective analysis of 213 patients Blood 99 3 840 9 doi 10 1182 blood V99 3 840 PMID 11806985 S2CID 1310629 FDA Approves New Therapy for Myelodysplastic Syndromes MDS That Can Be Taken at Home U S Food and Drug Administration FDA Press release 7 July 2020 Retrieved 7 July 2020 nbsp This article incorporates text from this source which is in the public domain Bacher U Haferlach T Schnittger S Kreipe H Kroger N March 2011 Recent advances in diagnosis molecular pathology and therapy of chronic myelomonocytic leukaemia Br J Haematol 153 2 149 67 doi 10 1111 j 1365 2141 2011 08631 x PMID 21401573 External links edit Retrieved from https en wikipedia org w index php title Chronic myelomonocytic leukemia amp oldid 1172818661, wikipedia, wiki, book, books, library,

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