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Chronic Monomyelocytic Leukemia (CMML)

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Manage episode 412557449 series 3565828
Innhold levert av Basics To Brilliance. Alt podcastinnhold, inkludert episoder, grafikk og podcastbeskrivelser, lastes opp og leveres direkte av Basics To Brilliance eller deres podcastplattformpartner. Hvis du tror at noen bruker det opphavsrettsbeskyttede verket ditt uten din tillatelse, kan du følge prosessen skissert her https://no.player.fm/legal.

Chronic MyeloMonocytic Leukemia (not CML)
Persistently high monocyte count- 3 months
Most frequent MDS/Myeloproliferative neoplasms – a cross between the two
Median age 72
Median survival 20-40 months
Transformation to AML (15-30%)

WHO definition of CMML:
1. Excess monocytes- persistent over 3 months, 1

- Monocytes 10% of total WC count
2. Dysplasia: morphological difference (blood film on BMBx)
OR
3. Genetic abnormalites ( on cytogenetics or molecular)

WHO Addition in 2022:
Persistent 3 months Monocytes 0.5 over 10% of WC count
AND Dysplasia
AND Genetic Abnormalities

No single diagnostic test

- Exclude MPNs: CML, MF, pre-fibrotic MF, PRV and ET
- Exclude Genetics: PDFGR A and B, FGFR 1, JAK-2 rearrangement
- Ensure less than 20% blasts

Common Presentation:
- Constitutional Sx
- Cytopenias and sequelae
- Effusions pericardial or pleural (inflammation and infiltration)
- Skin deposits
- Autoimmune disorders (higher incidence of CMML)

Classification:
-Myelodysplastic CMML- WC<13
o Cytopenias**

- Myeloproliferative CMML – WC 13
o Activate RAS pathway mutations
o Leukostasis**(*brain and lung*)
o More adverse clinical outcomes
o More splenomegaly and extra-medullary (infiltrative)
PROGNOSTIC CLASSIFICATION: Blast Count
- CMML-1: BMBx <10% blasts
- CMML-2: BMBx <20% blasts OR Presence of Auer Rods (trumps blast %)

OTHER:
o CPSS-Mol: cytogenetics, "NARS”, blast count, WBC count, transfusion dependence

Investigations
- R/O infection
- FBC and trend
- Blood film
- Flow of Peripheral blood (immunophenotyping): Chronic Panel
o Classical Monocyte MO1: CD14 +ve and CD16 -ve
- If >=94% MO1 on flow specific and sensitive for malignant
- Can help differentiate reactive monocytes MO3 (CD14 weak +ve, CD16 +ve)
-BMBx if appropriate as per age and fitness
o Aspirate: Dysplasia, Excess monocytes
o Flow: Acute panel (check blasts percentage)
o Cytogenetics:
- Poor cytogenetics: Trisomy 8, Chrom. 7 abnormalities, complex cytogenetics (3 or more cytogenetic abnormalities)
-Good cytogenetics: Isolated loss of chromosome Y
o Molecular: PCR in EDTA- “NARS”.....NRAS, ASXL1, RUNX1, SETBP1

Treatment decisions:
- High risk (AML risk) + Tx eligible -> Intensive chemo (AML style) and Tx
- Transplant outcomes: Overall survival approx. 30% but curable

- Low risk and not transplant eligible: QOL improvement
o Watch and wait
o Cytopenia supportive treatment w/ transfusions

o CMML-1 with raised WC count:
->Hydroxycarbimide as long as it provides benefit but can worsen cytopenias in patients with stable counts

o CMML-1 with significant cytopenias MML-2 with WC <13 with high risk of AML
-> Azacytidine (hypomethylating agent) Subcutaneous

  continue reading

5 episoder

Artwork
iconDel
 
Manage episode 412557449 series 3565828
Innhold levert av Basics To Brilliance. Alt podcastinnhold, inkludert episoder, grafikk og podcastbeskrivelser, lastes opp og leveres direkte av Basics To Brilliance eller deres podcastplattformpartner. Hvis du tror at noen bruker det opphavsrettsbeskyttede verket ditt uten din tillatelse, kan du følge prosessen skissert her https://no.player.fm/legal.

Chronic MyeloMonocytic Leukemia (not CML)
Persistently high monocyte count- 3 months
Most frequent MDS/Myeloproliferative neoplasms – a cross between the two
Median age 72
Median survival 20-40 months
Transformation to AML (15-30%)

WHO definition of CMML:
1. Excess monocytes- persistent over 3 months, 1

- Monocytes 10% of total WC count
2. Dysplasia: morphological difference (blood film on BMBx)
OR
3. Genetic abnormalites ( on cytogenetics or molecular)

WHO Addition in 2022:
Persistent 3 months Monocytes 0.5 over 10% of WC count
AND Dysplasia
AND Genetic Abnormalities

No single diagnostic test

- Exclude MPNs: CML, MF, pre-fibrotic MF, PRV and ET
- Exclude Genetics: PDFGR A and B, FGFR 1, JAK-2 rearrangement
- Ensure less than 20% blasts

Common Presentation:
- Constitutional Sx
- Cytopenias and sequelae
- Effusions pericardial or pleural (inflammation and infiltration)
- Skin deposits
- Autoimmune disorders (higher incidence of CMML)

Classification:
-Myelodysplastic CMML- WC<13
o Cytopenias**

- Myeloproliferative CMML – WC 13
o Activate RAS pathway mutations
o Leukostasis**(*brain and lung*)
o More adverse clinical outcomes
o More splenomegaly and extra-medullary (infiltrative)
PROGNOSTIC CLASSIFICATION: Blast Count
- CMML-1: BMBx <10% blasts
- CMML-2: BMBx <20% blasts OR Presence of Auer Rods (trumps blast %)

OTHER:
o CPSS-Mol: cytogenetics, "NARS”, blast count, WBC count, transfusion dependence

Investigations
- R/O infection
- FBC and trend
- Blood film
- Flow of Peripheral blood (immunophenotyping): Chronic Panel
o Classical Monocyte MO1: CD14 +ve and CD16 -ve
- If >=94% MO1 on flow specific and sensitive for malignant
- Can help differentiate reactive monocytes MO3 (CD14 weak +ve, CD16 +ve)
-BMBx if appropriate as per age and fitness
o Aspirate: Dysplasia, Excess monocytes
o Flow: Acute panel (check blasts percentage)
o Cytogenetics:
- Poor cytogenetics: Trisomy 8, Chrom. 7 abnormalities, complex cytogenetics (3 or more cytogenetic abnormalities)
-Good cytogenetics: Isolated loss of chromosome Y
o Molecular: PCR in EDTA- “NARS”.....NRAS, ASXL1, RUNX1, SETBP1

Treatment decisions:
- High risk (AML risk) + Tx eligible -> Intensive chemo (AML style) and Tx
- Transplant outcomes: Overall survival approx. 30% but curable

- Low risk and not transplant eligible: QOL improvement
o Watch and wait
o Cytopenia supportive treatment w/ transfusions

o CMML-1 with raised WC count:
->Hydroxycarbimide as long as it provides benefit but can worsen cytopenias in patients with stable counts

o CMML-1 with significant cytopenias MML-2 with WC <13 with high risk of AML
-> Azacytidine (hypomethylating agent) Subcutaneous

  continue reading

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